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Patent application title:

Template-fixed peptidomimetics with antimicrobial activity

Publication number:

-

Publication date:
Application number:

10/469,060

Filed date:

2002-02-18

βœ… Patent granted

Patent number:

US 7,253,146 B2

Grant date:

2007-08-07

PCT filing:

WO; PCT/EP02/01711; 20020218

PCT publication:

WO; WO02/070547; 20020912

Examiner:

Cecilia J. Tsang | Andrew D. Kosar

Adjusted expiration:

2022-02-18

Abstract:

Template-fixed Ξ²-hairpin peptidomimetics of the general formulae (I) and (II) wherein Z, Z1 and Z2 are template-fixed chains of 8 to 16 Ξ±-amino acid residues which, depending on their positions in the chain (counted starting from the N-terminal amino acid) are Gly, or Pro, or of certain types which, as the remaining symbols in the above formulae, are defined in the description and the claims, and salts thereof, have the property to inhibit the growth of or to kill microorganisms and cancer cells. They can be used as disinfectants for foodstuffs, cosmetics, medicaments or other nutrient-containing materials or as medicaments to treat or prevent infections or diseases related to such infections and/or cancer. These Ξ²-hairpin peptidomimetics can be manufactured by a process which is based on a mixed solid- and solution phase synthetic strategy

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Classification:

A61K38/12 IPC

Medicinal preparations containing peptides; Peptides having up to 20 amino acids in a fully defined sequence; Derivatives thereof Cyclic peptides, e.g. bacitracins; Polymyxins; Gramicidins S, C; Tyrocidins A, B or C

C07K5/12 IPC

Peptides containing up to four amino acids in a fully defined sequence; Derivatives thereof containing only normal peptide links Cyclic peptides with only normal peptide bonds in the ring

C07K2/00 IPC

Peptides of undefined number of amino acids; Derivatives thereof

C07K1/00 IPC

General methods for the preparation of peptides, i.e. processes for the organic chemical preparation of peptides or proteins of any length

A61K38/00 IPC

Medicinal preparations containing peptides

A61K38/02 IPC

Medicinal preparations containing peptides Peptides of undefined number of amino acids; Derivatives thereof

Description

CROSS-REFERENCE TO RELATED APPLICATIONS

This application is the national stage filing under 35 U.S.C. Β§371 of PCT/EP02/01711, filed Feb. 18, 2002, which claims priority to PCT/EP01/02072, filed Feb. 23, 2001, both of which are incorporated by reference.

BACKGROUND OF THE INVENTION

1. Field of the Invention

The present invention provides template-fixed Ξ²-hairpin peptidomimetics incorporating template-fixed chains of 8 to 16 Ξ±-amino acid residues which, depending on their positions in the chains, are Gly or Pro, or of certain types, as defined hereinbelow. These template-fixed Ξ²-hairpin mimetics have broad spectrum antimicrobial and anticancer activity. In addition, the present invention provides an efficient synthetic process by which these compounds can, if desired, be made in parallel library-format. These Ξ²-hairpin peptidomimetics show improved efficacy, bioavailability, half-life and most importantly a significantly enhanced ratio between antibacterial and anticancer activity on the one hand, and hemolysis of red blood cells on the other.

2. Description of Relevant Art

The growing problem of microbial resistance to established antibiotics has stimulated intense interest in developing novel antimicrobial agents with new modes of action (H. Breithaupt, Nat. Biotechnol. 1999, 17, 1165–1169). One emerging class of antibiotics is based on naturally occurring cationic peptides (T. Ganz, R. L. Lehrer, Mol. Medicine Today 1999, 5, 292–297; R. M. Epand, H. J. Vogel, Biochim. Biophys. Acta 1999, 1462, 11–28). These include disulfide-bridged Ξ²-hairpin and Ξ²-sheet peptides (such as the protegrins [V. N. M.; O. V. Shamova, H. A. Korneva, R. I. Lehrer, FEBS Lett. 1993, 327, 231–236], tachyplesins [T. Nakamura, H. Furunaka, T. Miyata, F. Tokunaga, T. Muta, S. Iwanaga, M. Niwa, T. Takao, Y. Shimonishi, Y. J. Biol. Chem. 1988, 263, 16709–16713], and the defensins [R. I. Lehrer, A. K. Lichtenstein, T. Ganz, Annu. Rev. Immunol. 1993, 11, 105–128], amphipathic Ξ±-helical peptides (e.g. cecropins, dermaseptins, magainins, and mellitins [A. Tossi, L. Sandri, A. Giangaspero, Biopolymers 2000, 55, 4–30]), as well as other linear and loop-structured peptides. Although the mechanisms of action of antimicrobial cationic peptides are not yet fully understood, their primary site of interaction is the microbial cell membrane (H. W. Huang, Biochemistry 2000, 39, 8347–8352). Upon exposure to these agents, the cell membrane undergoes permeabilization, which is followed by rapid cell death. However, more complex mechanisms of action, for example, involving receptor-mediated signaling; cannot presently be ruled out (M. Wu, E. Maier, R. Benz, R. E. Hancock, Biochemistry 1999, 38, 7235–7242).

The antimicrobial activities of many of these cationic peptides usually correlate with their preferred secondary structures, observed either in aqueous solution or in membrane-like environments (N. Sitaram, R. Nagaraj, Biochim. Biophys. Acta 1999, 1462, 29–54). Structural studies by nuclear magnetic resonance (NMR) spectroscopy have shown that cationic peptides such as protegrin 1 (A. Aumelas, M. Mangoni, C. Roumestand, L. Chiche, E. Despaux, G. Grassy, B. Calas, A. Chavanieu, A. Eur. J. Biochem. 1996, 237, 575–583; R. L. Fahrner, T. Dieckmann, S. S. L. Harwig, R. I. Lehrer, D. Eisenberg, J. Feigon, J. Chem. Biol. 1996, 3, 543–550) and tachyplesin I (K. Kawano, T. Yoneya, T. Miyata, K. Yoshikawa, F. Tokunaga, Y. Terada, S. J. Iwanaga, S. J. Biol. Chem. 1990, 265, 15365–15367) adopt well defined Ξ²-hairpin conformations, due to the constraining effect of two disulfide bridges. In protegrin analogues lacking one or both of these disulfide bonds, the stability of the Ξ²-hairpin conformation is diminished, and the antimicrobial activity is reduced (J. Chen, T. J. Falla, H. J. Liu, M. A. Hurst, C. A. Fujii, D. A. Mosca, J. R. Embree D. J. Loury, P. A. Radel, C. C. Chang, L. Gu, J. C. Fiddes, Biopolymers 2000, 55, 88–98; S. L. Harwig, A. Waring, H. J. Yang, Y. Cho, L. Tan, R. I. Lehrer, R. J. Eur. J. Biochem. 1996, 240, 352–357; M. E. Mangoni, A. Aumelas, P. Charnet, C. Roumestand, L. Chiche, E. Despaux, G. Grassy, B. Calas, A. Chavanieu, FEBS Lett. 1996, 383, 93–98; H. Tamamura, T. Murakami, S. Noriuchi, K. Sugihara, A. Otaka, W. Takada, T. Ibuka, M. Waki, N. Tamamoto, N. Fujii, Chem. Pharm. Bull. 1995, 43, 853–858). Similar observations have been made in analogues of tachyplesin I (H. Tamamura, R. Ikoma, M. Niwa, S. Funakoshi, T. Murakami, N. Fujii, Chem. Pharm. Bull. 1993, 41, 978–980) and in hairpin-loop mimetics of rabbit defensin NP-2 (S. Thennarasu, R. Nagaraj, Biochem. Biophys. Res. Comm. 1999, 254, 281–283). These results show that the Ξ²-hairpin structure plays an important role in the antimicrobial activity and stability of these protegrin-like peptides. In the case of the cationic peptides preferring Ξ±-helical structures, the amphililic structure of the helix appears to play a key role in determining antimicrobial activity (A. Tossi, L. Sandri, A. Giangaspero, A. Biopolymers 2000, 55, 430). Gramicidin S is a backbone-cyclic peptide with a well defined Ξ²-hairpin structure (S. E. Hull, R. Karlsson, P. Main, M. M. Woolfson, E. J. Dodson, Nature 1978, 275, 206–275) that displays potent antimicrobial activity against gram-positive and gram-negative bacteria (L. H. Kondejewski, S. W. Farmer, D. S. Wishart, R. E. Hancock, R. S. Hodges, Int. J. Peptide Prot. Res. 1996, 47, 460–466). The high hemolytic activity of gramicidin S has, however, hindered its widespread use as an antibiotic. Recent structural studies by NMR have indicated that the high hemolytic activity apparently correlates with the highly amphipathic nature of this cyclic Ξ²-hairpin-like molecule, but that it is possible to dissociate antimicrobial and hemolytic activities by modulating the conformation and amphiphilicity (L. H. Kondejewski, M. Jelokhani-Niarali, S. W. Farmer, B. Lix, M. Kay, B. D. Sykes, R. E. Hancock, R. S. Hodges, J. Biol. Chem. 1999, 274, 13181–13192; C. McInnes L. H. Kondejewski, R. S. Hodges, B. D. Sykes, J. Biol. Chem. 2000, 275, 14287–14294).

A new cyclic antimicrobial peptide RTD-1 was reported recently from primate leukocytes (Y.-Q. Tang, J. Yuan, G. Γ–sapay, K. Γ–sapay, D. Tran, C. J. Miller, A. J. Oellette, M. E. Selsted, Science 1999, 286, 498–502. This peptide contains three disulfide bridges, which act to constrain the cyclic peptide backbone into a hairpin geometry. Cleavage of the three disulfide bonds leads to a significant loss of antimicrobial activity. Analogues of protegrins (J. P. Tam, C. Wu, J.-L. Yang, Eur. J. Biochem. 2000, 267, 3289–3300) and tachyplesins (J.-P. Tam, Y.-A. Lu, I.-L. Yang, Biochemistry 2000, 39, 7159–7169; N. Sitaram, R. Nagaraij, Biochem. Biophys. Res. Comm. 2000, 267, 783–790) containing a cyclic peptide backbone, as well as multiple disulfide bridges to enforce a amphiphilic hairpin structure, have also been reported. In these cases, removal of all the cystine constraints does not always lead to a large loss of antimicrobial activity, but does modulate the membranolytic selectivity (J. P. Tam, C. Wu, J.-L. Yang, Eur. J. Biochem. 2000, 267, 3289–3300).

A key issue in the design of new cationic antimicrobial peptides is selectivity. The naturally occurring protegrins and tachyplesins exert a significant hemolytic activity against human red blood cells. This is also the case for protegrin analogues such as IB367 (J. Chen, T. J. Falla, H. J. Liu, M. A. Hurst, C. A. Fujii, D. A. Mosca, J. R. Embree, D. J. Loury, P. A. Radel, C. C. Chang, L. Gu, J. C. Fiddes, Biopolymers 2000, 55, 88–98; C. Chang, L. Gu, J. Chen, U.S. Pat. No. 5,916,872, 1999). This high hemolytic activity essentially obviates its use in vivo, and represents a serious disadvantage in clinical applications. Also, the antibiotic activity of analogues often decreases significantly with increasing salt concentration, such that under in vivo conditions (ca. 100–150 mM NaCl) the antimicrobial activity may be severely reduced. Before intravenous use can be considered, the general toxicity, protein-binding activity in blood serum, as well as protease stability become serious issues which must be adequately addressed.

Protegrin 1 exhibits potent and similar activity against gram-positive and gram-negative bacteria as well as fungi in both low- and high-salt assays. This broad antimicrobial activity combined with a rapid mode of action, and their ability to kill bacteria resistant to other classes of antibiotics, make them attractive targets for development of clinically useful antibiotics. The activity against gram-positive bacteria is typically higher than against gram-negative bacteria. However, protegrin 1 also exhibits a high hemolytic activity against human red blood cells, and hence a low selectivity towards microbial cells. Oriented CD experiments (W. T. Heller, A. J. Waring, R. I. Lehrer, H. W. Huang, Biochemistry 1998, 37, 17331–17338) indicate that protegrin 1 may exist in two different states as it interacts with membranes, and these states are strongly influenced by lipid composition. Studies of cyclic protegrin analogues (J.-P. Tam, C. Wu, J.-L. Yang, Eur. J. Biochem. 2000, 267, 3289–3300) have revealed, that an increase in the conformational rigidity, resulting from backbone cyclization and multiple disulfide bridges, may confer membranolytic selectivity that dissociates antimicrobial activity from hemolytic activity, at least in the series of compounds studied. Protegrin 1 is an 18 residues linear peptide, with an amidated carboxyl terminus and two disulfide bridges. Tachyplesin I contains 17 residues, also has an amidated carboxyl terminus and contains two disulfide bridges. Recently described backbone-cyclic protegrin and tachyplesin analogues typically contain 18 residues and up to three disulfide bridges (J. P. Tam, C. Wu, J.-L. Yang, Eur. J. Biochem. 2000, 267, 3289–3300; J. P. Tam, Y.-A. Lu, J.-L. Yang, Biochemistry 2000, 39, 7159–7169; N. Sitaram, R. Nagaraij, Biochem. Biophys. Res. Comm. 2000, 267, 783–790).

Cathelicidin, a 37-residue linear helical-type cationic peptide, and analogues are currently under investigation as inhaled therapeutic agents for cystic fibrosis (CF) lung disease (L. Saiman, S. Tabibi, T. D. Starner, P. San Gabriel, P. L. Winokur, H. P. Jia, P. B. McGray, Jr., B. F. Tack, Antimicrob. Agents and Chemother. 2001, 45, 2838–2844; R. E. W. Hancock, R. Lehrer, Trends Biotechnol. 1998, 16, 82–88). Over 80% of CF patients become chronically infected with pseudomonas aeruginosa (C. A. Demko, P. J. Biard, P. B. Davies, J. Clin. Epidemiol. 1995, 48, 1041–1049; E. M. Kerem, R. Gold, H. Levinson, J. Pediatr. 1990, 116, 714–719).

In addition, there is evidence from the literature that some cationic peptides exibit interesting anticancer activity. Cerecropin B, a 35-residue Ξ±-helical cationic peptide isolated from the hemolymph of the giant silk moth, and shorter analogues derived from Cerecropin B have been investigated as potential anticancer compounds (A. J. Moore, D. A. Devine, M. C. Bibby, Peptide Research 1994, 7, 265–269).

SUMMARY OF THE INVENTION

In the compounds described below, a new strategy is introduced to stabilize Ξ²-hairpin conformations in backbone-cyclic cationic peptide mimetic exhibiting antimicrobial and anticancer activity. This involves transplanting the cationic and hydrophobic hairpin sequence onto a template, whose function is to restrain the peptide loop backbone into a hairpin geometry. The rigidity of the hairpin may be further influenced by introducing a disulfide bridge. The template moiety may also act as an attachment point for other organic groups, that may modulate the antimicrobial and/or membranolytic targeting selectivity of the molecule, and be useful for producing dimeric species, where the templates in each monomer unit are linked through a short spacer or linker. Template-bound hairpin mimetic peptides have been described in the literature (D, Obrecht, M. Altorfer, J. A. Robinson, Adv. Med. Chem. 1999, 4, 1–68; J. A. Robinson, Syn. Lett. 2000, 4, 429–441), but such molecules have not previously been evaluated for development of antimicrobial peptides. However, the ability to generate Ξ²-hairpin peptidomimetics using combinatorial and parallel synthesis methods has now been established (L. Jiang, K. Moehle, B. Dhanapal, D. Obrecht, J. A. Robinson, Helv. Chim. Acta. 2000, 83, 3097–3112).

These methods allow the synthesis and screening of large hairpin mimetic libraries, which in turn considerably facilitates structure-activity studies, and hence the discovery of new molecules with potent antimicrobial and anticancer activity and low hemolytic activity to human red blood cells. Furthermore, the present strategy allows to synthesize Ξ²-hairpin peptidomimetics with novel selectivities towards different types of pathogens, e.g. towards various multi-rug resistant pseudomonas strains. Ξ²-Hairpin peptidomimetics obtained by the approach described here can be used amongst other applications, e.g. as broad spectrum antibiotics, as therapeutics for cystic fibrosis lung disease and anticancer agents.

The Ξ²-hairpin peptidomimetics of the present invention are compounds of the general formulae


wherein


is a group of one of the formulae


wherein


is the residue of an L-Ξ±-amino acid with B being a residue of formula β€”NR20CH(R71)β€” or the enantiomer of one of the groups A1 to A69 as defined hereinafter;


is a group of one of the formulae

  • R1 is H; lower alkyl; or aryl-lower allyl;
  • R2 is H; allyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R3 is H; allyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R4 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)p(CHR61)sCOOR57; β€”(CH2)p(CHR61)sCONR58R59; β€”(CH2)p(CHR61)sPO(OR60)2; β€”(CH2)p(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R5 is alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R6 is H; alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R7 is alkyl; alkenyl; β€”(CH2)q(CHR61)sOR55; β€”(CH2)q(CHR61)sNR33R34; β€”(CH2)q(CHR61)sOCONR33R75; β€”(CH2)q(CHR61)sNR20CONR33R82; β€”(CH2)r(CHR61)sCOOR57; β€”(CH2)r(CHR61)sCONR58R59; β€”(CH2)r(CHR61)sPO(OR60)2; β€”(CH2)r(CHR61)sSO2R62; or β€”(CH2)r(CHR61)sC6H4R8;
  • R8 is H; Cl; F; CF3; NO2; lower alkyl; lower alkenyl; aryl; aryl-lower alkyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sCOR64;
  • R9 is alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R10 is alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R11 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R69; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC5H4R8;
  • R12 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)rCHR61)sCOOR57; β€”(CH2)r(CHR61)sCONR58R59; β€”(CH2)r(CHR61)sPO(OR60)2; β€”(CH2)r(CHR61)sSO2R62; or β€”(CH2)rCHR61)sC6H4R8;
  • R13 is alkyl; alkenyl; β€”(CH2)q(CHR61)sOR55; β€”(CH2)q(CHR61)sSR56; β€”(CH2)q(CHR61)sNR33R34; β€”(CH2)q(CHR61)sOCONR33R75; β€”(CH2)q(CHR61)sNR20CONR33R82; β€”(CH2)q(CHR61)sCOOR57; β€”(CH2)q(CHR61)sCONR58R59; β€”(CH2)q(CHR61)sPO(OR60)2; β€”(CH2)q(CHR61)sSO2R62; or β€”(CH2)q(CHR61)sC6H4R8;
  • R14 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)q(CHR61)sCOOR57; β€”(CH2)q(CHR61)sCONR58R59; β€”(CH2)q(CHR61)sPO(OR60)2; β€”(CH2)q(CHR61)sSOR62; or β€”(CH2)q(CHR61)sC6H4R8;
  • R15 is alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)q(CHR61)s SO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R16 is alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R17 is alkyl; alkenyl; β€”(CH2)q(CHR61)sOR55; β€”(CH2)q(CHR61)sSR56; β€”(CH2)q(CHR61)sNR33R34; β€”(CH2)q(CHR61)sOCONR33R75; β€”(CH2)q(CHR61)sNR20CONR33R82; β€”(CH2)q(CHR61)sCOOR57; β€”(CH2)q(CHR61)sCONR58R59; β€”(CH2)q(CHR61)sPO(OR60)2; β€”(CH2)q(CHR61)sSO2R62; or β€”(CH2)q(CHR61)sC6H4R8;
  • R18 is alkyl; alkenyl; β€”(CH2)p(CHR61)sOR55; β€”(CH2)p(CHR61)sSR56; β€”(CH2)p(CHR61)sNR33R34; β€”(CH2)p(CHR61)sOCONR33R75; β€”(CH2)p(CHR61)sNR20CONR33R82; β€”(CH2)p(CHR61)sCOOR57; β€”(CH2)p(CHR61)sCONR58R59; β€”(CH2)p(CHR61)sPO(OR60)2; β€”(CH2)p(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R19 is lower alkyl; β€”(CH2)p(CHR61)sOR55; β€”(CH2)p(CHR61)sSR56; β€”(CH2)p(CHR61)sNR33R34; β€”(CH2)p(CHR61)sOCONR33R75; β€”(CH2)p(CHR61)sNR20CONR33R82; β€”(CH2)p(CHR61)sCOOR57; β€”(CH2)p(CHR61)sCONR58R59; β€”(CH2)p(CHR61)sPO(OR60)2; β€”(CH2)p(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8; or
  • R18 and R19 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;
  • R20 is H; alkyl; alkenyl; or aryl-lower alkyl;
  • R21 is H; alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R22 is H; alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R23 is alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R24 is alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61))sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R25 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R26 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8; or
  • R25 and R26 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)rO(CH2)rβ€”; β€”(CH2)rS(CH2)rβ€”; or β€”(CH2)rR57(CH2)rβ€”;
  • R27 is H; alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R28 is alkyl; alkenyl; β€”(CH2)o(CHR61)sβ€”OR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)s(CHR61)sC6H4R8;
  • R29 is alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)s SO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R30 is H; alkyl; alkenyl; or aryl-lower alkyl;
  • R31 is H; alkyl; alkenyl; β€”(CH2)p(CHR61)sOR55; β€”(CH2)p(CHR61)sNR33R34; β€”(CH2)p(CHR61)sOCONR33R75; β€”(CH2)p(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R32 is H; lower alkyl; or aryl-lower alkyl;
  • R33 is H; alkyl, alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sNR34R63; β€”(CH2)m(CHR61)sOCONR75R82; β€”(CH2)m(CHR61)sNR20CONR78R82; β€”(CH2)o(CHR61)sCOR64; β€”(CH2)o(CHR61)sβ€”CONR58R59, β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R34 is H; lower alkyl; aryl, or aryl-lower alkyl;
  • R33 and R34 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;
  • R35 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)p(CHR61)sCOOR57; β€”(CH2)p(CHR61)sCONR58R59; β€”(CH2)p(CHR61)sPO(OR60)2; β€”(CH2)p(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R36 is H, alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)p(CHR61)sNR33R34; β€”(CH2)p(CHR61)sOCONR33R75; β€”(CH2)p(CHR61)sNR20CONR33R82; β€”(CH2)p(CHR61)sCOOR57; β€”(CH2)p(CHR61)sCONR58R59; β€”(CH2)p(CHR61)sPO(OR60)2; β€”(CH2)p(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R37 is H; F; Br, Cl; NO2; CF3; lower alkyl; β€”(CH2)p(CHR61)sOR55; β€”(CH2)p(CH61)sNR33R34; β€”(CH2)p(CHR61)sOCONR33R75; β€”(CH2)p(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R38 is H; F; Br; Cl; NO2; CF3; alkyl; alkenyl; β€”(CH2)p(CHR61)sOR55; β€”(CH2)p(CHR61)sNR33R34; β€”(CH2)p(CHR61)sOCONR33R75; β€”(CH2)p(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R39 is H; alkyl; alkenyl; or aryl-lower alkyl;
  • R40 is H; alkyl; alkenyl; or aryl-lower alkyl;
  • R41 is H; F; Br; Cl; NO2; CF3; alkyl; alkenyl; β€”(CH2)p(CHR61)sOR55; β€”(CH2)p(CHR61)sNR33R34; β€”(CH2)p(CHR61)sOCONR33R75; β€”(CH2)p(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R42 is H; F; Br, Cl; NO2; CF3; alkyl; alkenyl; β€”(CH2)p(CHR61)sOR55; β€”(CH2)p(CHR61)sNR33R34; β€”(CH2)p(CHR61)sOCONR33R75; β€”(CH2)p(CHR61)sNR20CONR35R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R43 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R44 is alkyl; alkenyl; β€”(CH2)r(CHR61)sOR55; β€”(CH2)r(CHR61)sSR56; β€”(CH2)r(CHR61)sNR33R34; β€”(CH2)r(CHR61)sOCONR33R75; β€”(CH2)r(CHR61)sNR20CONR33R82; β€”(CH2)r(CHR61)sCOOR57; β€”(CH2)r(CHR61)sCONR58R59; β€”(CH2)r(CHR61)sPO(OR60)2; β€”(CH2)r(CHR61)sSO2R62; or β€”(CH2)r(CHR61)sC6H4R8;
  • R45 is H; alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)s(CHR61)sCONR58R59; β€”(CH2)s(CHR61)sPO(OR60)2; β€”(CH2)s(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;
  • R46 is H; alkyl; alkenyl; or β€”(CH2)o(CHR61)pC6H4R8;
  • R47 is H; alkyl; alkenyl; or β€”(CH2)o(CHR61)sOR55;
  • R48 is H; lower alkyl; lower alkenyl; or aryl-lower alkyl;
  • R49 is H; alkyl; alkenyl; β€”(CHR61)sCOOR57; (CHR61)sCONR58R59; (CHR61)sPO(OR60)2; β€”(CHR61)sSOR62; or β€”(CHR61)sC6H4R8;
  • R50 is H; lower alkyl; or aryl-lower allyl;
  • R57 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)pPO(OR60)2; β€”(CH2)p(CHR61)sSO2R62; or β€”(CH2)p(CHR61)sC6H4R8;
  • R52 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)pPO(OR60)2; β€”(CH2)p(CHR61)sSO2R62; or β€”(CH2)p(CHR61)sC6H4R8;
  • R53 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)pPO(OR60)2; β€”(CH2)p(CHR61)sSO2R62; or β€”(CH2)p(CHR61)sC6H4R8;
  • R54 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)COOR57; β€”(CH2)o(CHR61)sCONR58R59; or β€”(CH2)o(CHR61)sC6H4R8;
  • R55 is H; lower alkyl; lower alkenyl; aryl-lower alkyl; β€”(CH2)m(CHR61)sOR57; β€”(CH2)m(CHR61)sNR34R63; β€”(CH2)m(CHR61)sOCONR75R82; β€”(CH2)m(CHR61)sNR20CONR78R82; β€”(CH2)o(CHR61)sβ€”COR64; β€”(CH2)o(CHR61)COOR57; or β€”(CH2)o(CHR61)sCONR58R59;
  • R56 is H; lower alkyl; lower alkenyl; aryl-lower allyl; β€”(CH2)m(CHR61)sOR57; β€”(CH2)m(CHR61)sNR34R63; β€”(CH2)m(CHR61)sOCONR75R82; β€”(CH2)m(CHR61)sNR20CONR78R82; β€”(CH2)o(CHR61)sβ€”COR64; or β€”(CH2)o(CHR61)sCONR58R59;
  • R57 is H; lower alkyl; lower alkenyl; aryl lower alkyl; or heteroaryl lower alkyl;
  • R58 is H; lower alkyl; lower alkenyl; aryl; heteroaryl; aryl-lower alkyl; or heteroaryl-lower alkyl;
  • R59 is H; lower alkyl; lower alkenyl; aryl; heteroaryl; aryl-lower alkyl; or heteroaryl-lower alkyl; or
  • R58 and R59 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;
  • R60 is H; lower alkyl; lower alkenyl; aryl; or aryl-lower alkyl;
  • R61 is alkyl; alkenyl; aryl; heteroaryl; aryl-lower alkyl; heteroaryl-lower alkyl; β€”(CH2)mOR55; β€”(CH2)mNR33R34; β€”(CH2)mOCONR75R82; β€”(CH2)mNR20CONR78R82; β€”CH2)oCOOR37; β€”(CH2)oR58R59; or β€”(CH2)oPO(COR60)2;
  • R62 is lower alkyl; lower alkenyl; aryl, heteroaryl; or aryl-lower alkyl;
  • R63 is H; lower alkyl; lower alkenyl; aryl, heteroaryl; aryl-lower alkyl; heteroaryl-lower alkyl; β€”COR64; β€”COOR57; β€”CONR58R59; β€”SO2R62; or β€”PO(OR60)2;
  • R34 and R63 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;
  • R64 is H; lower alkyl; lower alkenyl; aryl; heteroaryl; aryl-lower alkyl; heteroaryl-lower alkyl; β€”(CH2)p(CHR61)sOR65; β€”(CH2)p(CHR61)sSR66; or β€”(CH2)p(CHR61)sNR34R63; β€”(CH2)p(CHR61)sOCONR75R82; β€”(CH2)p(CHR61)sNR20CONR78R82;
  • R65 is H; lower alkyl; lower alkenyl; aryl, aryl-lower alkyl; heteroaryl-lower alkyl; β€”COR57; β€”COOR57; or β€”CONR58R59;
  • R65 is H; lower alkyl; lower alkenyl; aryl; aryl-lower alkyl; heteroaryl-lower alkyl; or β€”CONR58R59;
  • m is 2–4; o is 0–4; p is 1–4; q is 0–2; r is 1 or 2; s is 0 or 1;


independently have any of the significances defined above for


except (a1) or (a2) with B being β€”NR20CH(R71)β€” and with A being A80, A81, A90, A91, A95 or A96, and except (f) and (m), but wherein

  • R2 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R3 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R4 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)m(CHR61)sNR3β€”; or β€”(CH2)p(CHR61)sCOβ€”;
  • R5 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R6 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R7 is β€”(CH2)q(CHR61)sOβ€”; β€”(CH2)q(CHR61)sNR34; or β€”(CH2)r(CHR61)sCOβ€”;
  • R8 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R9 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R10 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R11 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R12 is β€”(CH2)m(CHR61)sOβ€”, β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)r(CHR61)sCOβ€”;
  • R13 is β€”(CH2)q(CHR61)sOβ€”; β€”(CH2)q(CHR61)sSβ€”; β€”(CH2)q(CHR61)sNR34β€”; or β€”(CH2)q(CHR61)sCOβ€”;
  • R14 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)q(CHR61)sCOβ€”;
  • R15 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R16 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R17 is β€”(CH2)q(CHR61)sOβ€”; β€”(CH2)q(CHR61)sSβ€”; β€”(CH2)q(CHR61)sNR34β€”; or β€”(CH2)q(CHR61)sCOβ€”;
  • R18 is β€”(CH2)p(CHR61)sOβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)p(CHR61)sNR34β€”; or β€”(CH2)p(CHR61)sCOβ€”;
  • R19 is β€”(CH2)p(CHR61)sOβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)p(CHR61)sNR34β€”; or β€”(CH2)p(CHR61)sCOβ€”;
  • R21 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R22 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R23 is β€”(CH2)o(CHR61)sO; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R24 is β€”(CH2)o(CHR61)sO; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R25 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R26 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R27 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”, β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R28 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sNR34; or β€”(CH2)o(CHR61)sCOβ€”;
  • R29 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R31 is β€”(CH2)p(CHR61)sOβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)p(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R33 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CH2)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R37 is β€”(CH2)p(CHR61)sOβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)p(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R38 is β€”(CH2)p(CHR61)sOβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)p(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R41 is β€”(CH2)p(CHR61)sOβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)p(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R42 is β€”(CH2)p(CHR61)sOβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)p(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R43 is β€”(CH2)m(CHR61)sO; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R45 is β€”(CH2)o(CHR61)sOβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)o(CHR61)sNR34β€”; or β€”(CH2)s(CHR61)sCOβ€”;
  • R47 is β€”(CH2)o(CHR61)sOβ€”;
  • R49 is β€”(CHR61)sOβ€”; β€”(CHR61)sSβ€”; β€”(CHR61)sNR34β€”; or β€”(CHR61)sCOβ€”;
  • R51 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R52 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R53 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R54 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R55 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R56 is β€”(CH2)m(CHR61)sOβ€”; β€”(CH2)m(CHR61)sNR34β€”; or β€”(CH2)o(CHR61)sCOβ€”;
  • R64 is β€”(CH2)p(CHR61)sOβ€”; β€”(CH2)p(CHR61)sSβ€”; or β€”(CH2)p(CHR61)sNR34β€”;
  • m, o, p, q, r and s being as defined above;
  • with the proviso that if more than one of the substituents R2 to R19, R21 to R19, R31, R33, R37, R38, R41 to R43, R45, R47, R49, R51 to R56 and R64 is present, only one of these has one of the significances just mentioned whilst the other(s) has/have any of the significance(s) mentioned earlier;
  • L is a direct bond or one of the linkers
  • L1: β€”(CH2)pCHR61[X(CH2)pCHR61]oβ€”;
  • L2: β€”CO(CH2)pCHR61[X(CH2)pCHR61]oCOβ€”;
  • L3: β€”CONR34(CH2)pCHR61[X(CH2)pCHR61]oNR34COβ€”;
  • L4: β€”O(CH2)pCHR61[X(CH2)pCHR61]oOβ€”;
  • L5: β€”S(CH2)pCHR61[X(CH2)pCHR61]oSβ€”;
  • L6: β€”NR34(CH2)pCHR61[X(CH2)pCHR61]oNR34β€”;
  • L7: β€”(CH2)oCHR61Y(CH2)oCHR61β€”;
  • L8: β€”CO(CH2)oCHR61Y(CH2)oCHR61COβ€”;
  • L9: β€”CONR34(CH2)oCHR61Y(CH2)oCHR61NR34COβ€”;
  • L10: β€”O(CH2)oCHR61Y(CH2)oCHR61Oβ€”;
  • L11: β€”S(CH2)oCHR61Y(CH2)oCHR61Sβ€”;
  • L12: β€”NR34(CH2)oCHR61Y(CH2)oCHR61NR34β€”;
  • L13: β€”CO(CH2)pCHR61[X(CH2)pCHM61]oNR34β€”;
  • L14: β€”CO(CH2)oCHR61Y(CH2)oCHR61NR34β€”;
  • L15 β€”NR34(CH2)pCHR61[X(CH2)pCHR61]oCOβ€”; and
  • L16 β€”NR34(CH2)oCHR61Y(CH2)oCHR61COβ€”;
  • m, o, p, q, r and s being as defined above; X being O; S; NR34; β€”NR32CONR34β€”; or β€”OCOOβ€”; and Y being β€”C6R67R68R69R70β€”;
  • R67 being H; Cl; Br; F; NO2; β€”NR34COR57; lower alkyl; or lower alkenyl;
  • R68 being H; Cl; Br; F; NO2; β€”NR34COR57; lower alkyl; or lower alkenyl;
  • R69 being H; Cl; Br; F; NO2; β€”NR34COR57; lower alkyl; or lower alkenyl; and
  • R70 being H; Cl; Br, F; NO2; β€”NR34COR57; lower alkyl; or lower alkenyl;
  • with the proviso that at least two of R67, R68, R69 and R70 are H; and
  • with the further proviso that
  • β€”(CH2)m(CHR61)sOβ€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)o(CHR61)sOβ€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)p(CHR61)sOβ€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)q(CHR61)sOβ€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CHR61)sOβ€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)m(CHR61)sSβ€” can be combined with linker L1, L2, L3, L7, L8 or L9; or can form a disulfide bond with β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CHR2)q(CHR61)sSβ€”; or β€”(CHR61)sSβ€”;
  • β€”(CH2)o(CHR61)sSβ€” can be combined with linker L1, L2, L3, L7, L8 or L9; or can form a disulfide bond with β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)q(CHR61)sSβ€”; or β€”(CHR61)sSβ€”;
  • β€”(CH2)p(CHR61)sSβ€” can be combined with linker L1, L2, L3, L7, L8 or L9; or can form a disulfide bond with β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)q(CHR61)sSβ€”; or β€”(CHR61)sSβ€”;
  • β€”(CH2)q(CHR61)sSβ€” can be combined with linker L1, L2, L3, L7, L8 or L9; or can form a disulfide bond with β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)q(CHR61)sSβ€”; or β€”(CHR61)sSβ€”;
  • β€”(CHR61)sSβ€” can be combined with linker L1, L2, L3, L7, L8 or L9; or form a disulfide bond with β€”(CH2)m(CHR61)sSβ€”; β€”(CH2)o(CHR61)sSβ€”; β€”(CH2)p(CHR61)sSβ€”; β€”(CH2)q(CHR61)sSβ€”; or β€”(CHR61)sSβ€”;
  • β€”(CH2)m(CHR61)sNR34β€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)o(CHR61)sNR34β€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)p(CHR61)sNR34β€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)q(CHR61)sNR34β€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CHR61)sNR34β€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)o(CHR61)sCOβ€” can be combined with linker L4, L5, L6, L1, L11 or L12;
  • β€”(CH2)p(CHR61)sCOβ€” can be combined with linker L4, L5, L6, L1, L11 or L12;
  • β€”(CH2)q(CHR61)sCOβ€” can be combined with linker L4, L5, L6, L10, L11 or L12;
  • β€”(CH2)r(CHR61)sCOβ€” can be combined with linker L4, L5, L6, L10, L11 or L12;
  • β€”(CHR61)sCOβ€” can be combined with linker L4, L5, L6, L10, L11 or L12;
  • β€”(CH2)m(CHR61)sOβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)m(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)o(CHR61)sOβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)p(CHR61)sCOβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)q(CHR61)sOβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CHR61)sOβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)m(CHR61)sSβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)o(CHR61)sSβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)p(CHR61)sSβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)q(CHR61)sSβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CHR61)sSβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)m(CHR61)sNR34β€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”, β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)o(CHR61)sNR34β€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)p(CHR61)sNR34β€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)q(CHR61)sNR34β€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CHR61)sNR34β€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)o(CHR61)sCOβ€”; β€”(CH2)o(CHR61)pCOβ€”; β€”(CH2)q(CHR61)sCOβ€”; or β€”(CHR61)sCOβ€”;
  • β€”(CH2)o(CHR61)sCOβ€” can be combined with linker L15 or L16 and the resulting combination with β€”(CH2)m(CHR61)sXβ€”, β€”(CH2)o(CHR61)sXβ€”, β€”(CH2)p(CHR61)sXβ€”, β€”(CH2)q(CHR61)sXβ€”; or β€”(CHR61)sXβ€”;
  • β€”(CH2)p(CHR61)sCOβ€” can be combined with linker L15 or L16 and the resulting combination with β€”(CH2)m(CHR61)sXβ€”, β€”(CH2)o(CHR61)sXβ€”, β€”(CH2)p(CHR61)sXβ€”, β€”(CH2)q(CHR61)sXβ€”; or β€”(CHR61)sXβ€”;
  • β€”(CH2)q(CHR61)sCOβ€” can be combined with linker L15 or L16 and the resulting combination with β€”(CH2)m(CHR61)sXβ€”, β€”(CH2)o(CHR61)sXβ€”, β€”(CH2)p(CHR61)sXβ€”, β€”(CH2)q(CHR61)sXβ€”; or β€”(CHR61)sXβ€”;
  • β€”(CH2)r(CHR61)sCOβ€” can be combined with linker L15 or L16 and the resulting combination with β€”(CH2)m(CHR61)sXβ€”, β€”(CH2)o(CHR61)sXβ€”, β€”(CH2)p(CHR61)sXβ€”, β€”(CH2)q(CHR61)sXβ€”; or β€”(CHR61)sXβ€”;
  • β€”(CHR61)sCOβ€” can be combined with linker L15 or L16 and the resulting combination with β€”(CH2)m(CHR61)sXβ€”; β€”(CH2)o(CHR61)sXβ€”; β€”(CH2)p(CHR61)sXβ€”; β€”(CH2)q(CHR61)sXβ€”; or β€”(CHR61)sXβ€”;
  • Z, Z1 and Z2 independently are chains of n Ξ±-amino acid residues, n being an integer from 8 to 16, the positions of said amino acid residues in said chains being counted starting from the N-terminal amino acid, whereby these amino acid residues are, depending on their position in the chains, Gly, or Pro, or of formula -A-COβ€”, or of formula β€”Bβ€”COβ€”, or of one of the types
  • C: β€”NR20CH(R72)COβ€”;
  • D: β€”NR20CH(R73)COβ€”;
  • E: β€”NR20CH(R74)COβ€”;
  • F: β€”NR20CH(R84)COβ€”; and
  • H: β€”NR20β€”(CH(COβ€”)β€”(CH2)4-7β€”(CH(COβ€”)β€”NR20β€”; β€”NR20β€”CH(COβ€”)β€”(CH2)pSS(CH2)pβ€”(CH(COβ€”)β€”NR20β€”; β€”NR20β€”CH(COβ€”)β€”(CH2)pNR20CO(CH2)pβ€”CH(COβ€”)β€”NR20β€”; and β€”NR20β€”(CH(COβ€”)β€”(β€”(CH2)pNR20CONR20(CH2)pβ€”(CH(COβ€”)β€”NR20β€”;
  • R71 is H; lower alkyl; lower alkenyl; β€”(CH2)p(CHR61)sOR75; β€”(CH2)p(CHR61)sSR75; β€”(CH2)p(CHR61)sNR33R34; β€”(CH2)p(CHR61)sOCONR33R75; β€”(CH2)p(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR75; β€”(CH2)pCONR58R59; β€”(CH2)pPO(OR62)2; β€”(CH2)pSO2R62; or β€”(CH2)oβ€”C6R67R68R69R70R76;
  • R72 is H; lower alkyl; lower alkenyl; β€”(CH2)p(CHR61)sOR85; or β€”(CH2)p(CHR61)sSR85;
  • R73 is β€”(CH2)oR77; β€”(CH2)rO(CH2)oR77; β€”(CH2)rS(CH2)oR77; or β€”(CH2)rNR20(CH2)oR77;
  • R74 is β€”(CH2)pNR78R79; β€”(CH2)pNR77R80; β€”(CH2)pC(═NR80)NR78R79; β€”(CH2)pC(═NOR50)NR78R79; β€”(CH2)pC(═NNR78R79)NR78R79; β€”(CH2)pNR80C(═NR80)NR78R79; β€”(CH2)pN═C(NR78R80)NR79R80; β€”(CH2)pC6H4NR78R79; β€”(CH2)pC6H4NR77R80; β€”(CH2)pC6H4C(═NR80)NR78R79; β€”(CH2)pC6H4C(═NOR50)NR78R79; β€”(CH2)pC6H4C(═NNR78R79)NR78R79; β€”(CH2)pC6H4NR80C(═NR80)NR78R79; β€”(CH2)pC6H4N═C(NR78R80)NR79NR80; β€”(CH2)rO(CH2)mNR78R79; β€”(CH2)rO(CH2)mNR77R80; β€”(CH2)rO(CH2)pC(═NR80)NR78R79; β€”(CH2)rO(CH2)pC(═NOR50)NR78R79; β€”(CH2)rO(CH2)pC(═NNR78R79)NR78R79; β€”(CH2)rO(CH2)mNR80C(═NR80)NR78R79; β€”(CH2)rO(CH2)mN═C(NR78R80)NR79R80; β€”(CH2)rO(CH2)pC6H4CNR78R79; β€”(CH2)rO(CH2)pC6H4C(═NR80)NR78R79; β€”(CH2)rO(CH2)pC6H4C(═NOR50)NR78R79; β€”(CH2)rO(CH2)pC6H4C(═NNR78R79)NR78R79; β€”(CH2)rO(CH2)pC6H4NR80C(═NR80)NR78R79; β€”(CH2)rS(CH2)mNR78R79; β€”(CH2)rS(CH2)mNR77R80; β€”(CH2)rS(CH2)pC(═NR80)NR78R79; β€”(CH2)rS(CH2)pC(═NOR50)NR78R79; β€”(CH2)rS(CH2)pC(═NNR78R79)NR78R79; β€”(CH2)rS(CH2)mNR80C(═NR80)NR78R79; β€”(CH2)rS(CH2)mN═C(NR78R80)NR79R80; β€”(CH2)rS(CH2)pC6H4CNR78R79; β€”(CH2)rS(CH2)pC6H4C(β€”NR80)NR78R79; β€”(CH2)rS(CH2)pC6H4C(═NOR50)NR78R79; β€”(CH2)rS(CH2)pC6H4C(═NNR78R79)NR78R79; β€”(CH2)rS(CH2)pC6H4NR80C(═NR80)NR78R79; β€”(CH2)pNR80COR64; β€”(CH2)pNR80COR77; β€”(CH2)pNR80CONR78R79; or β€”(CH2)pC6H4NR80CONR78R79;
  • R75 is lower alkyl; lower alkenyl; or aryl-lower allyl;
  • R33 and R75 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;
  • R75 and R82 taken together can form β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;
  • R76 is H; lower alkyl; lower alkenyl; aryl-lower alkyl; β€”(CH2)oOR72; β€”(CH2)oSR72; β€”(CH2)oNR33R34; β€”(CH2)oOCONR33R75; β€”(CH2)oNR20CONR33R82; β€”(CH2)oCOOR75; β€”(CH2)oCONR58R59; β€”(CH2)oPO(OR60)2; β€”(CH2)pSO2R62; or β€”(CH2)oCOR64;
  • R77 is β€”C6R67R68R69R70R76; or a heteroaryl group of one of the formulae

  • R78 is H; lower alkyl; aryl; or aryl-lower alkyl;
  • R78 and R82 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;
  • R79 is H; lower alkyl; aryl; or aryl-lower alkyl; or
  • R78 and R79, taken together, can be β€”(CH2)2-7β€”; β€”(CH2)2O(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;
  • R80 is H; or lower alkyl;
  • R81 is H; lower alkyl; or aryl-lower alkyl;
  • R82 is H; lower alkyl; aryl; heteroaryl; or aryl-lower alkyl;
  • R33 and R82 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;
  • R83 is H; lower allyl; aryl; or β€”NR78R79;
  • R84 is β€”(CH2)m(CHR61)sOH; β€”(CH2)pCONR78R79; β€”(CH2)pNR80CONR78R79; β€”(CH2)pC6H4CONR78R79; or β€”(CH2)pC6H4NR80CONR78R79;
  • R85 is lower alkyl; or lower alkenyl;
  • with the proviso that in said chain(s) of n Ξ±-amino acid residues Z, Z1 and Z2
    • if n is 8, the amino acid residues in positions 1 to 8 are:
      • P1: of type C or of type D or of type E or of type F, or the residue is Pro;
      • P2: of type E or of type D or of type F;
      • P3: of type E or of type C, or the residue is Pro;
      • P4: of type E or of formula -A-COβ€”;
      • P5: of type E or of formula β€”Bβ€”COβ€”, or the residue is Gly;
      • P6: of type D, or the residue is Pro;
      • P7: of type or of type C or of type D; and
      • P8: of type C or of type D or of type E or of type F, or the residue is Pro; or
      • P2 and P7, taken together, can form a group of type H; and at P4 and P5 also D-isomers being possible;
    • if n is 9, the amino acid residues in positions 1 to 9 are:
      • P1: of type C or of type D or of type E or of type F, or the residue is Pro;
      • P2: of type E or of type D or of type F;
      • P3: of type C or of type D or of type E, or the residue is Pro;
      • P4: of type E or of type D, or the residue is Pro;
      • P5: of type E, or the residue is Gly or Pro;
      • P6: of type D or of type E, or the residue is Gly or Pro;
      • P7: of type E or of type D or of type C, or the residue is Pro;
      • P8: of type E or of type D; and
      • P9: of type C or of type D or of type E or of type F, or the residue is Pro; or
      • P2 and P8, taken together, can form a group of type H; and at P4, P5 and P6 also D-isomers being possible;
    • if n is 10, the amino acid residues in positions 1 to 10 are:
      • P1: of type C or of type D or of type E or of type F, or the residue is Pro;
      • P2: of type E or of type D, or the residue is Pro;
      • P3: of type C or of type E;
      • P4: of type E or of type D or of type F, or the residue is Pro;
      • P5: of type E or of type F or of formula -A-COβ€”, or the residue is Gly;
      • P6: of type E or of formula β€”Bβ€”COβ€”, or the residue is Gly;
      • P7: of type D or of type E, or the residue is Gly or Pro;
      • P8: of type D or of type E;
      • P9: of type E or of type D or of type C, or the residue is Pro; and
      • P10: of type C or of type D or of type E or of type F; or
      • P3 and P8, taken together, can form a group of type H; and at P5 and P6 also D-isomers being possible;
    • if n is 11, the amino acid residues in positions 1 to 11 are:
      • P1: of type C or of type D or of type E or of type F, or the residue is Pro;
      • P2: of type E or of type C or of type D;
      • P3: of type D or of type E, or the residue is Pro;
      • P4: of type E or of type C or of type F;
      • P5: of type E or of type F, or the residue is Gly or Pro;
      • P6: of type E or of type F, or the residue is Gly or Pro;
      • P7: of type E or of type F, or the residue is Gly or Pro;
      • P8: of type D or of type E or of type F;
      • P9: of type D or of type E, or the residue is Pro;
      • P10: of type E or of type C or of type D; and
      • P11: of type C or of type D or of type E or of type F, or the residue is Pro; or
      • P4 and P8 and/or P2 and P10, taken together, can form a group of type H; and at P5, P6 and P7 also D-isomers being possible;
    • if n is 12, the amino acid residues in positions 1 to 12 are:
      • P1: of type C or of type D or of type E or of type F, or the residue is Pro;
      • P2: of type E or of type D;
      • P3: of type C or of type D, or the residue is Pro;
      • P4: of type E or of type F or of type D;
      • P5: of type E or of type D or of type C, or the residue is Gly or Pro;
      • P6: of type E or of type F or of formula -A-COβ€”, or the residue is Gly;
      • P7: of type E or of type F or of formula β€”Bβ€”COβ€”;
      • P8: of type D or of type C, or the residue is Pro;
      • P9: of type E or of type D or of type F;
      • P10: of type D or of type C, or the residue is Pro;
      • P11: of type E or of type D; and
      • P12: of type C or of type D or of type E or of type F, or the residue is Pro; or
      • P4 and P9 and/or P2 and P11, taken together, can form a group of type H; and
      • at P6 and P7 also D-isomers being possible;
    • if n is 13, the amino acid residues in positions 1 to 13 are:
      • P1: of type C or of type D or of type E or of type F, or the residue is Pro;
      • P2: of type E or of type F or of type D;
      • P3: of type C or of type D or of type E, or the residue is Pro;
      • P4: of type E of type C or of type F;
      • P5: of type E or of type D, or the residue is Gly or Pro;
      • P6: of type B or of type F, or the residue is Gly or Pro;
      • P7: of type E or of type F, or the residue is Pro;
      • P8: of type D or of type E or of type F, or the residue is Pro;
      • P9: of type D or of type E, or the residue is Pro;
      • P10: of type E or of type C or of type F;
      • P11: of type C or of type E, or the residue is Pro;
      • P12: of type E or of type D or of type C; and
      • P13: of type C or of type D or of type E or of type F, or the residue is Pro; or P4 and P10 and/or P2 and P12, taken together, can form a group of type H; and at P6, P7 and P8 also D-isomers being possible;
    • if n is 14, the amino acid residues in positions 1 to 14 are:
      • P1: of type C or of type D or of type E or of type F, or the residue is Pro;
      • P2: of type E or of type C or of type D, or the residue is Pro;
      • P3: of type C or of type D or of type E;
      • P4: of type D or of type C or of type E, or the residue is Pro;
      • P5: of type E or of type D;
      • P6: of type E or of type F, or the residue is Gly or Pro;
      • P7: of type E or of type F or of formula -A-COβ€”, or the residue is Gly;
      • P8: of type E or of type F or of formula β€”Bβ€”COβ€”, or the residue is Gly;
      • P9: of type D or of type E, or the residue is Pro;
      • P10: of type C or of type D or of type E;
      • P11: of type E or of type D or of type F, or the residue is Pro;
      • P12: of type D or of type E;
      • P13: of type E or of type C or of type D, or the residue is Pro; and
      • P14: of type C or of type D or of type E or of type F, or the residue is Pro; or
      • P5 and P10 and/or P3 and P12, taken together, can form a group of type H; and at P7 and P8 also D-isomers being possible;
    • if n is 15, the amino acid residues in positions 1 to 15 are:
      • P1: of type C or of type D or of type E or of type F, or the residue is Pro;
      • P2: of type E or of type F or of type D;
      • P3: of type C or of type D or of type E, or the residue is Pro;
      • P4: of type E or of type D or of type F;
      • P5: of type C or of type D or of type E, or the residue is Pro;
      • P6: of type E or of type D or of type F;
      • P7: of type C or of type E, or the residue is Pro;
      • P8: of type E or of type F, or the residue is Gly or Pro;
      • P9: of type E or of type F, or the residue is Gly or Pro;
      • P10: of type E or of type D;
      • P11: of type C or of type D or of type E, or the residue is Pro;
      • P12: of type E or of type C or of type F;
      • P13: of type D or of type E, or the residue is Pro;
      • P14: of type E or of type C or of type D; and
      • P15: of type C or of type D or of type E or of type F, or the residue is Pro; or
    • P6 and P10 and/or P4 and P12 and/or P2 and P14, taken together, can form a group of type H; and at P7, P8 and P9 also D-isomers being possible; and
    • if n is 16, the amino acid residues in positions 1 to 16 are:
      • P1: of type D, or of type E or of type C or of type F, or the residue is Pro;
      • P2: of type E or of type F or of type D;
      • P3: of type C or of type D or of type E, or the residue is Pro;
      • P4: of type E or of type D or of type F;
      • P5: of type D or of type C or of type E, or the residue is Pro;
      • P6: of type E or of type D;
      • P7: of type E or of type F, or the residue is Gly or Pro;
      • P8: of type E or of type F or of formula -A-COβ€”, or the residue is Gly;
      • P9: of type E or of formula β€”Bβ€”COβ€”, or the residue is Gly;
      • P10: of type D or of type E, or the residue is Pro;
      • P11: of type E or of type C or of type D;
      • P12: of type D or of type C or of type E, or the residue is Pro;
      • P13; of type E or of type C or of type F;
      • P14: of type C or of type D or of type E, or the residue is Pro;
      • P15: of type E or of type C or of type D; and
      • P16: of type C or of type D or of type E or of type F, or the residue is Pro; or
      • P6 and P11 and/or P4 and P13 and/or P2 and P15, taken together, can form a group of type H; and at P8 and P9 also D-isomers being possible;
        and pharmaceutically acceptable salts thereof.

In accordance with the present invention these Ξ²-hairpin peptidomimetics can be prepared by a process which comprises

  • (a) coupling an appropriately functionalized solid support with an appropriately N-protected derivative of that amino acid which in the desired end-product is in position n/2, n/2+1 or n/2βˆ’1 if n is an even number and, respectively, in position n/2+Β½ or n/2βˆ’Β½ if n is an odd number, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;
  • (b) removing the N-protecting group from the product thus obtained;
  • (c) coupling the product thus obtained with an appropriately N-protected derivative of that amino acid which in the desired end-product is one position nearer the N-terminal amino acid residue, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;
  • (d) removing the N-protecting group from the product thus obtained;
  • (e) repeating, if necessary, steps (c) and (d) until the N-terminal amino acid residue has been introduced;
  • (f) coupling the product thus obtained to a compound of the general formula


wherein


is as defined above and X is an N-protecting group or, if


is to be group (a1) or (a2), above, alternatively

    • (fa) coupling the product obtained in step (d) or (e) with an appropriately N-protected derivative of an amino acid of the general formula
      HOOCβ€”Bβ€”H  III
      or
      HOOC-A-H  IV
    • wherein B and A are as defined above, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;
    • (fb) removing the N-protecting group from the product thus obtained; and
    • (fc) coupling the product thus obtained with an appropriately N-protected derivative of an amino acid of the above general formula IV and, respectively, III, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;
  • (g) removing the N-protecting group from the product obtained in step (f) or (fc);
  • (h) coupling the product thus obtained to an appropriately N-protected derivative of that amino acid which in the desired end-product is in position n, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;
  • (i) removing the N-protecting group from the product thus obtained;
  • (j) coupling the product thus obtained to an appropriately N-protected derivative of that amino acid which in the desired end-product is one position farther away from position n, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;
  • (k) removing the N-protecting group from the product thus obtained;
  • (l) repeating, if necessary, steps (j) and (k) until all amino acid residues have been introduced;
  • (m) if desired, selectively deprotecting one or several protected functional group(s) present in the molecule and appropriately substituting the reactive group(s) thus liberated;
  • (o) detaching the product thus obtained from the solid support;
  • (p) cyclizing the product cleaved from the solid support;
  • (q) if, desired
    • (qa) forming one or several interstrand linkage(s) between side-chains of appropriate amino acid residues at opposite positions of the Ξ²-stand region; and/or
    • (qb) connecting two building blocks of the type of formula Ia via a bridge -G1-L-G2-;
  • (r) removing any protecting groups present on functional groups of any members of the chain of amino acid residues and, if desired, any protecting group(s) which may in addition be present in the molecule; and
  • (s) if desired, converting the product thus obtained into a pharmaceutically acceptable salt or converting a pharmaceutically acceptable, or unacceptable, salt thus obtained into the corresponding free compound of formula I or into a different, pharmaceutically acceptable, salt.

The peptidomimetics of the present invention can also be enantiomers of the compounds of formulae Ia and Ib. These enantiomers can be prepared by a modification of the above process in which enantiomers of all chiral starting materials are used.

DETAILED DESCRIPTION OF THE INVENTION

As used in this description, the term β€œalkyl”, taken alone or in combinations, designates saturated, straight-chain or branched hydrocarbon radicals having up to 24, preferably up to 12, carbon atoms. Similarly, the term β€œalkenyl” designates straight chain or branched hydrocarbon radicals having up to 24, preferably up to 12, carbon atoms and containing at least one or, depending on the chain length, up to four olefinic double bonds. The term β€œlower” designates radicals and compounds having up to 6 carbon atoms. Thus, for example, the term β€œlower alkyl” designates saturated, straight-chain or branched hydrocarbon radicals having up to 6 carbon atoms, such as methyl, ethyl, n-propyl, isopropyl, n-butyl, sec.-butyl, isobutyl, tert.-butyl and the like. The term β€œaryl” designates aromatic carbocyclic hydrocarbon radicals containing one or two six-membered rings, such as phenyl or naphthyl, which may be substituted by up to three substituents such as Br, Cl, F, CF3, NO2, lower alkyl or lower alkenyl. The term β€œheteroaryl” designates aromatic heterocyclic radicals containing one or two five- and/or six-membered rings, at least one of them containing up to three heteroatoms selected from the group consisting of O, S and N and said ring(s) being optionally substituted; representative examples of such optionally substituted heteroaryl radicals are indicated hereinabove in connection with the definition of R77.

The structural element -A-COβ€” designates amino acid building blocks which in combination with the structural element β€”Bβ€”COβ€” form templates (a1) and (a2). Templates (a) through (p) constitute building blocks which have an N-terminus and a C-terminus oriented in space in such a way that the distance between those two groups may lie between 4.0–5.5 A. A peptide chain Z, Z1 or Z2 is linked to the C-terminus and the N-terminus of the templates (a) through (p) via the corresponding N- and C-termini so that the template and the chain form a cyclic structure such as that depicted in formula Ia. In a case as here where the distance between the N- and C-termini of the template lies between 4.0–5.5 A the template will induce the H-bond network necessary for the formation of a Ξ²-hairpin conformation in the peptide chain Z, Z1 or Z2. Thus template and peptide chain form a Ξ²-hairpin mimetic. The Ξ²-hairpin mimetics can also be coupled through groups G1 and G2 and a linker unit L to form the dimeric constructs of formula Ib.

The Ξ²-hairpin conformation is highly relevant for the antibiotic and anticancer activities of the Ξ²-hairpin mimetics of the present invention. The Ξ²-hairpin stabilizing conformational properties of the templates (a) through (p) play a key role not only for antibiotic and anticancer activity but also for the synthesis process defined hereinabove, as incorporation of the templates near the middle of the linear protected peptide precursors enhance significantly cyclization yields.

Building blocks A1–A69 belong to a class of amino acids wherein the N-terminus is a secondary amine forming part of a ring. Among the genetically encoded amino acids only proline falls into this class. The configuration of building block A1 through A69 is (D), and they are combined with a building block β€”Bβ€”COβ€” of (L)-configuration. Preferred combinations for templates (a1) are-DA1-CO-LB-COβ€” to DA69-CO-LB-COβ€”. Thus, for example, DPro-LPro constitutes the prototype of templates (a1). Less preferred, but possible are combinations where templates (a2) are -LA1-CO-DB-COβ€” to LA69-CO-DBCOβ€”. Thus, for example, LPro-DPro constitutes a less preferred prototype of template (a2).

It will be appreciated that building blocks -A1-COβ€” to -A69-COβ€” in which A has (D)-configuration, are carrying a group R1 at the Ξ±-position to the N-terminus. The preferred values for R1 are H and lower alkyl with the most preferred values for R1 being H and methyl. It will be recognized by those skilled in the art, that A1–A69 are shown in (D)-configuration which, for R1 being H and methyl, corresponds to the (R)-configuration. Depending on the priority of other values for R1 according to the Cahn, Ingold and Prelog-rules, this configuration may also have to be expressed as (S).

In addition to R1 building blocks -A1-COβ€” to -A69-COβ€” can carry an additional substituent designated as R2 to R17. This additional substituent can be H, and if it is other than H, it is preferably a small to medium-sized aliphatic or aromatic group. Examples of preferred values for R2 to R17 are:

    • R2: H; lower alkyl; lower alkenyl; (CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower allyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64(where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R3: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”, where R57: H; or lower alkyl); β€”(CH2)o(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R4: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mS56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R5: lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; R57: where H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: alkyl; alkenyl; aryl; and aryl-lower alkyl; heteroaryl-lower alkyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R6: H; lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R7: lower alkyl; lower alkenyl; β€”(CH2)qOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)qSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)qNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)qOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); (CH2)qNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)qN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)rCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)qCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)rPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)rSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R9: lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR5, (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower allyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”, β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R10: lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”, or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R11: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R12: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)rCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)rCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)rPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R13: lower alkyl; lower alkenyl; β€”(CH2)qOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)qSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)qNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)qOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)qNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)qN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)rCOO57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)qCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)rPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)rSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R14: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R15: lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); particularly favoured are NR20CO lower alkyl (R20=H; or lower alkyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R16: lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R17: lower alkyl; lower alkenyl; β€”(CH2)qOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)qSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)qNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)qOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)qNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)qN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)rCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)qCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)rPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)rSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).

Among the building blocks A1 to A69 the following are preferred: A5 with R2 being H, A8, A22, A25, A38 with R2 being H, A42, A47, and A50. Most preferred are building blocks of type A8β€²:


wherein R20 is H or lower alkyl; and R64 is alkyl; alkenyl; aryl; aryl-lower alkyl; or heteroaryl-lower alkyl; especially those wherein R64 is n-hexyl (A8β€²-1); n-heptyl (A8β€²-2); 4-(phenyl)benzyl (A8β€²-3); diphenylmethyl (A8β€²-4); 3-amino-propyl (A8β€²-5); 5-amino-pentyl (A8β€²-6); methyl (A8β€²-7); ethyl (A8β€²-8); isopropyl (A8β€²-9); isobutyl (A8β€²-10); n-propyl (A8β€²-11); cyclohexyl (A8β€²-12); cyclohexylmethyl (A8β€²-13); n-butyl (A8β€²-14); phenyl (A8β€²-15); benzyl (A8β€²-16); (3-indolyl)methyl (A8β€²-17); 2-(3-indolyl)ethyl (A8β€²-18); (4-phenyl)phenyl (A8β€²-19); and n-nonyl (A8β€²-20).

Building block A70 belongs to the class of open-chained Ξ±-substituted Ξ±-amino acids, building blocks A71 and A72 to the corresponding Ξ²-amino acid analogues and building blocks A73–A104 to the cyclic analogues of A70. Such amino acid derivatives have been shown to constrain small peptides in well defined reverse turn or U-shaped conformations (C. M. Venkatachalam, Biopolymers, 1968, 6, 1425–1434; W. Kabsch, C Sander, Biopolymers 1983, 22, 2577). Such building blocks or templates are ideally suited for the stabilization of Ξ²-hairpin conformations in peptide loops (D. Obrecht, M. Altorfer, J. A. Robinson, β€œNovel Peptide Mimetic Building Blocks and Strategies for Efficient Lead Finding”, Adv. Med Chem. 1999, Vol. 4, 1–68; P. Balaram, β€œNon-standard amino acids in peptide design and protein engineering”, Curr. Opin. Struct. Biol. 1992, 2, 845–851; M. Crisma, G. Valle, C. Toniolo, S. Prasad, R. B. Rao, P. Balaram, β€œΞ²-turn conformations in crystal structures of model peptides containing Ξ±,Ξ±-disubstituted amino acids”, Biopolymers 1995, 35, 1–9; V. J. Hruby, F. Al-Obeidi, W. Kazmierski, Biochem. J. 1990, 268, 249–262).

It has been shown that both enantiomers of building blocks -A70-COβ€” to A104-COβ€” in combination with a building block β€”Bβ€”COβ€” of L-configuration can efficiently stabilize and induce Ξ²-hairpin conformations (D. Obrecht, M. Altorfer, J. A. Robinson, β€œNovel Peptide Mimetic Building Blocks and Strategies for Efficient Lead Finding”, Adv. Med Chem 1999, Vol. 4, 1–68; D. Obrecht, C. Spiegler, P. Schorholm, K. MΓΌller, H. Heimgartner, F. Stierli, Helv. Chin. Acta 1992, 75, 1666–1696; D. Obrecht, U. Bohdal, J. Daly, C. Lehmann, P. SchΓΆnholzer, K. MΓΌller, Tetrahedron 1995, 51, 10883–10900; D. Obrecht, C. Lehmann, C. Ruffieux, P. SchΓΆnholzer, K. MΓΌller, Helv. Chim. Acta 1995, 78, 1567–1587; D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580; D. Obrecht, H. Karajiannis, C. Lehmann, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 703–714).

Thus, for the purposes of the present invention templates (a1) can also consist of -A70-COβ€” to A104-COβ€” where building block A70 to A104 is of either (D)- or (L)-configuration, in combination with a building block β€”Bβ€”COβ€” of (L)-configuration.

Preferred values for R20 in A70 to A104 are H or lower alkyl with methyl being most preferred. Preferred values for R18, R19 and R21–R29 in building blocks A70 to A104 are the following:

    • R18: lower alkyl.
    • R19: lower alkyl; lower alkenyl; β€”(CH2)pOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)pSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)pNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)pCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)pCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)pSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)oC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R21: H; lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or (CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R22: lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF; lower alkyl; lower alkenyl; or lower alkoxy).
    • R23: H; lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); particularly favoured are NR20CO lower alkyl (R20=H; or lower alkyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3, lower alkyl; lower alkenyl; or lower alkoxy);
    • R24: lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); particularly favoured are NR20CO lower alkyl (R20=H ; or lower alkyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy);
    • R25: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R26: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • Alternatively. R25 and R26 taken together can be β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl).
    • R27: H; lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R28: lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R29: lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)oCOR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); particularly favored are NR20CO lower-alkyl (R20=H; or lower alkyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).

For templates (b) to (p), such as (b1) and (c1), the preferred values for the various symbols are the following:

    • R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)sR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; or lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R20: H; or lower alkyl.
    • R30: H, methyl.
    • R31: H; lower alkyl; lower alkenyl; β€”(CH2)pOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)pNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); (β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)rC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy); most preferred is β€”CH2CONR58R59 (R58: H; or lower alkyl; R59: lower alkyl; or lower alkenyl).
    • R32: H, methyl.
    • R33: lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mNR34R63 (where R34: lower alkyl; or lower alkenyl; R63: H; or lower alkyl; or R34 and R63 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); (CH2)mOCONR75R82 (where R75: lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R75 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR78R82 (where R20: H; or lower lower alkyl; R78: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R78 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl).
    • R34: H; or lower alkyl.
    • R35: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl).
    • R36: lower alkyl; lower alkenyl; or aryl-lower alkyl.
    • R37: H; lower alkyl; lower alkenyl; β€”(CH2)pOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)pNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pNR20CONR33R82 (where R20: H; or lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R38: H; lower alkyl; lower alkenyl; β€”(CH2)pOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)pNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R82 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R39: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl).
    • R40: lower alkyl; lower alkenyl; or aryl-lower alkyl.
    • R41: H; lower alkyl; lower alkenyl; β€”(CH2)pOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)pNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”, β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6C4R8 (where R81: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R42: H; lower alkyl; lower alkenyl; β€”(CH2)pOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)pNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”, where R57: H; or lower alkyl); β€”(CH2)pNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl, or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R43: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60: lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62: lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R44: lower alkyl; lower alkenyl; β€”(CH2)pOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)pSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)pNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R78 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”, β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)pN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)pCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)pCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); or β€”(CH2)oC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R45: H; lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)oNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)sOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”, β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); or β€”(CH2)sC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R46: H; lower alkyl; lower alkenyl; β€”(CH2)sOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)sSR56 (where R56: lower alkyl; or lower alkenyl); β€”(CH2)sNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)sOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)sNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)sN(R20)oCOR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”, or β€”(CH2)2NR57(CH2)β€”; where R57: H; or lower alkyl); or β€”(CH2)sC6H4R3 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R47: H; or OR55 (where R55: lower alkyl; or lower alkenyl).
    • R48: H; or lower alkyl.
    • R49: H; lower alkyl; β€”(CH2)oCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); or (CH2)sC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R50: H; methyl.
    • R51: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R3: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); (CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)pCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)pCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); or β€”(CH2)rC6H4R8 (where R85: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R52: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)pCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)pCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); or β€”(CH2)rC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R53: H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55: lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33: lower alkyl; or lower alkenyl; R34: H; or lower alkyl; or R33 and R34 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33: H; or lower alkyl; or lower alkenyl; R75: lower alkyl; or R33 and R75 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20: H; or lower lower alkyl; R33: H; or lower alkyl; or lower alkenyl; R82: H; or lower alkyl; or R33 and R82 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); β€”(CH2)mN(R20)COR64 (where: R20: H; or lower alkyl; R64: lower alkyl; or lower alkenyl); β€”(CH2)pCOOR57 (where R57: lower alkyl; or lower alkenyl); β€”(CH2)pCONR58R59 (where R58: lower alkyl; or lower alkenyl; and R59: H; lower alkyl; or R58 and R59 taken together form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57: H; or lower alkyl); or β€”(CH2)rC6H4R8 (where R8: H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).
    • R54: lower alkyl; lower alkenyl; or aryl-lower alkyl.

Among the building blocks A70 to A104 the following are preferred: A74 with R22 being H, A75, A76, A77 with R22 being H, A78 and A79.

The building block β€”Bβ€”COβ€” within template (a1) and (a2) designates an L-amino acid residue. Preferred values for B are: β€”NR20CH(R71)β€” and enantiomers of groups A5 with R2 being H, A8, A22, A25, A38 with R2 being H, A42, A47, and A50. Most preferred are
Ala L-Alanine
Arg L-Arginine
Asn L-Asparagine
Cys L-Cysteine
Gln L-Glutamine
Gly Glycine
His L-Histidine
Ile L-Isoleucine
Leu L-Leucine
Lys L-Lysine
Met L-Methionine
Phe L-Phenylalanine
Pro L-Proline
Ser L-Serine
Thr L-Threonine
Trp L-Tryptophan
Tyr L-Tyrosine
Val L-Valine
Cit L-Citrulline
Orn L-Ornithine
tBuA L-t-Butylalanine
Sar Sarcosine
t-BuG L-tert.-Butylglycine
4AmPhe L-para-Aminophenylalanine
3AmPhe L-meta-Aminophenylalanine
2AmPhe L-ortho-Aminophenylalanine
Phe(mC(NH2)═NH) L-meta-Amidinophenylalanine
Phe(pC(NH2)═NH) L-para-Amidinophenylalanine
Phe(mNHC (NH2)═NH) L-meta-Guanidinophenylalanine
Phe(pNHC (NH2)═NH) L-para-Guanidinophenylalanine
Phg L-Phenylglycine
Cha L-Cyclohexylalanine
C4al L-3-Cyclobutylalanine
C5al L-3-Cyclopentylalanine
Nle L-Norleucine
2-Nal L-2-Naphthylalanine
1-Nal L-1-Naphthylalanine
4Cl-Phe L-4-Chlorophenylalanine
3Cl-Phe L-3-Chlorophenylalanine
2Cl-Phe L-2-Chlorophenylalanine
3,4Cl2-Phe L-3,4-Dichlorophenylalanine
4F-Phe L-4-Fluorophenylalanine
3F-Phe L-3-Fluorophenylalanine
2F-Phe L-2-Fluorophenylalanine
Tic L-1,2,3,4-Tetrahydroisoquinoline-3-
carboxylic acid
Thi L-Ξ²-2-Thienylalanine
Tza L-2-Thiazolylalanine
Mso L-Methionine sulfoxide
AcLys L-N-Acetyllysine
Dpr L-2,3-Diaminopropionic acid
A2Bu L-2,4-Diaminobutyric acid
Dbu (S)-2,3-Diaminobutyric acid
Abu Ξ³-Aminobutyric acid (GABA)
Aha Ξ΅-Aminohexanoic acid
Aib Ξ±-Aminoisobutyric acid
Y(Bzl) L-O-Benzyltyrosine
Bip L-Biphenylalanine
S(Bzl) L-O-Benzylserine
T(Bzl) L-O-Benzylthreonine
hCha L-Homo-cyclohexylalanine
hCys L-Homo-cysteine
hSer L-Homo-serine
hArg L-Homo-arginine
hPhe L-Homo-phenylalanine
Bpa L-4-Benzoylphenylalanine
Pip L-Pipecolic acid
OctG L-Octylglycine
MePhe L-N-Methylphenylalanine
MeNle L-N-Methylnorleucine
MeAla L-N-Methylalanine
MeIle L-N-Methylisoleucine
MeVal L-N-Methvaline
MeLeu L-N-Methylleucine

In addition, the most preferred values for B also include groups of type A8β€³ of (L)-configuration:


wherein R20 is H or lower alkyl and R64 is alkyl; alkenyl; aryl; aryl-lower alkyl; or heteroaryl-lower alkyl; especially those wherein R64 is n-hexyl (A8β€³-21); n-heptyl (A8β€³-22); 4-(phenyl)benzyl (A8β€³-23); diphenylmethyl (A8β€³-24); 3-amino-propyl (A8β€³-25); 5-amino-pentyl (A8β€³-26); methyl (A8β€³-27); ethyl (A8β€³-28); isopropyl (A8β€³-29); isobutyl (A8β€³-30); n-propyl (A8β€³-31); cyclohexyl (A8β€³-32); cyclohexyhnethyl (A8β€³-33); n-butyl (A8β€³-34); phenyl (A8β€³-35); benzyl (A8β€³-36), (3-indolyl)methyl (A8β€³-37); 2-(3-indolyl)ethyl (A8β€³-38); (4-phenyl)phenyl (A8β€³-39); and n-nonyl (A8β€³-40).

The peptidic chains Z, Z1 and Z2 of the Ξ²-hairpin mimetics described herein are generally defined in terms of amino acid residues belonging to one of the following groups:

    • Group C β€”NR20CH(R72)COβ€”; β€œhydrophobic: small to medium-sized”
    • Group D β€”NR20CH(R73)COβ€”; β€œhydrophobic: large aromatic or heteroaromatic”
    • Group E β€”NR20CH(R74)COβ€”; β€œpolar-cationic”, β€œacylamino” and β€œurea-derived”
    • Group F β€”NR20CH(R84)COβ€”; β€œpolar-non-charged”
    • Group H β€”NR20β€”CH(COβ€”)β€”(CH2)4-7β€”CH(COβ€”)β€”NR20β€”; β€”NR20β€”CH(COβ€”)β€”(CH2)pSS(CH2)pβ€”CH(COβ€”)β€”NR20β€”; β€”NR20β€”CH(COβ€”)β€”(β€”(CH2)pNR20CO(CH2)p β€”CH(COβ€”)β€”NR20β€”; and β€”NR20β€”CH(COβ€”)β€”(β€”(CH2)pCONR20(CH2)pβ€”CH(COβ€”)β€”NR20β€”; β€œinterstrand linkage”

Furthermore, the amino acid residues in chains Z, Z1 and Z2 can also be of formula -A-COβ€” or of formula β€”Bβ€”COβ€” wherein A and B are as defined above. Finally, Gly can also be an amino acid residue in chains Z, Z1 and Z2, and Pro can be an amino acid residue in chains Z, Z1 and Z2, too, with the exception of positions where interstrand linkages (E) are possible.

Group C comprises amino acid residues with small to medium-sized hydrophobic side chain groups according to the general definition for substituent R72. A hydrophobic residue refers to an amino acid side chain that is uncharged at physiological pH and that is repelled by aqueous solution. Furthermore these side chains generally do not contain hydrogen bond donor groups, such as (but not limited to) primary and secondary amides, primary and secondary amines and the corresponding protonated salts thereof, thiols, alcohols, phosphonates, phosphates, ureas or thioureas. However, they may contain hydrogen bond acceptor groups such as ethers, thioethers, esters, tertiary amides, alkyl- or aryl phosphonates and phosphates or tertiary amines. Genetically encoded small-to-medium-sized amino acids include alanine, isoleucine, leucine, methionine and valine.

Group D comprises amino acid residues with aromatic and heteroaromatic side chain groups according to the general definition for substituent R73. An aromatic amino acid residue refers to a hydrophobic amino acid having a side chain containing at least one ring having a conjugated Ο€-electron system (aromatic group). In addition they may contain hydrogen bond donor groups such as (but not limited to) primary and secondary amides, primary and secondary amines and the corresponding protonated salts thereof, thiols, alcohols, phosphonates, phosphates, ureas or thioureas, and hydrogen bond acceptor groups such as (but not limited to) ethers, thioethers, esters, tetriary amides, alkylβ€”or aryl phosphonatesβ€”and phosphates or tertiary amines. Genetically encoded aromatic amino acids include phenylalanine and tyrosine.

A heteroaromatic amino acid residue refers to a hydrophobic amino acid having a side chain containing at least one ring having a conjugated Ο€-system incorporating at least one heteroatom such as (but not limited to) O, S and N according to the general definition for substituent R77. In addition such residues may contain hydrogen bond donor groups such as (but not limited to) primary and secondary amides, primary and secondary amines and the corresponding protonated salts thereof, thiols, alcohols, phosphonates, phosphates, ureas or thioureas, and hydrogen bond acceptor groups such as (but not limited to) ethers, thioethers, esters, tetriary amides, alkylβ€”or aryl phosphonates and phosphates or tertiary amines. Genetically encoded heteroaromatic amino acids include tryptophan and histidine.

Group E comprises amino acids containing side chains with polar-cationic, acylamino- and urea-derived residues according to the general definition for substituen R74. Polar-cationic refers to a basic side chain which is protonated at physiological pH. Genetically encoded polar-cationic amino acids include arginine, lysine and histidine. Citrulline is an example for an urea derived amino acid residue.

Group F comprises amino acids containing side chains with polar-non-charged residues according to the general definition for substituent R84. A polar-non-charged residue refers to a hydrophilic side chain that is uncharged at physiological pH, but that is not repelled by aqueous solutions. Such side chains typically contain hydrogen bond donor groups such as (but not limited to) primary and secondary amides, primary and secondary amines, thiols, alcohols, phosphonates, phosphates, ureas or thioureas. These groups can form hydrogen bond networks with water molecules. In addition they may also contain hydrogen bond acceptor groups such as (but not limited to) ethers, thioethers, esters, tetriary amides, alkyl- or aryl phosphonates and phosphates or tertiary amines. Genetically encoded polar-non-charged amino acids include asparagine, cysteine, glutamine, serine and threonine.

Group H comprises side chains of preferably (L)-amino acids at opposite positions of the Ξ²-strand region that can form an interstrand linkage. The most widely known linkage is the disulfide bridge formed by cysteines and homo-cysteines positioned at opposite positions of the Ξ²-strand. Various methods are known to form disulfide linkages including those described by: J. P. Tam et al. Synthesis 1979, 955–957; Stewart et al., Solid Phase Peptide Synthesis, 2d Ed., Pierce Chemical Company, III., 1984; Ahmed et al. J. Biol. Chem. 1975, 250, 8477–8482; and Pennington et al., Peptides, pages 164–166, Giralt and Andreu, Eds., ESCOM Leiden, The Netherlands, 1990. Most advantageously, for the scope of the present invention, disulfide linkages can be prepared as described hereinafter in the pertinent Examples (procedure 3), using acetamidomethyl (Acm)β€”protective groups for cysteine. A well established interstrand linkage consists in linking ornithines and lysines, respectively, with glutamic and aspartic acid residues located at opposite Ξ²-strand positions by means of an amide bond formation. Preferred protective groups for the side chain amino-groups of ornithine and lysine are alkyloxycarbonyl (Alloc) and alkylesters for aspartic and glutamic acid as described hereinafter in the pertinent Examples (procedure 4). Finally, interstrand linkages can also be established by linking the amino groups of lysine and omithine located at opposite Ξ²-strand positions with reagents such as N,N-arbonylimidazole to form cyclic ureas.

As mentioned earlier, positions for interstrand linkages are the following:

    • If n=8: Positions P2 and n taken together,
    • if n=9: Positions P2 and P8 taken together,
    • if n=10:Positions P3 and P8 taken together,
    • if n=11:Positions P4 and P8; and/or P2 and P10 taken together;
    • if n=12:Positions P4 and P9; and/or P2 and P11 taken together,
    • if n=13:Positions P4 and P10; and/or Positions P2 and P12 taken together;
    • if n=14:Positions P5 and P10; and/or P3 and P12 taken together; and
    • if n=15:Positions P6 and P10; and/or P4 and P12; and/or n and P14.
    • if n=16:Positions P6 and P11; and/or P4 and P13; and/or P2 and P15 taken together.

Such interstrand linkages are known to stabilize the Ξ²-hairpin conformations and thus constitute an important structural element for the design of Ξ²-hairpin mimetics.

Most preferred amino acid residues chains Z, Z1 and Z2 are those derived from natural Ξ±-amino acids. Hereinafter follows a list of amino acids which, or the residues of which, are suitable for the purposes of the present invention, the abbreviations corresponding to generally adopted usual practice:

three letter code one letter code
Ala L-Alanine A
Arg L-Arginine R
Asn L-Asparagine N
Asp L-Aspartic acid D
Cys L-Cysteine C
Glu L-Glutamic acid E
Gln L-Glutamine Q
Gly Glycine G
His L-Histidine H
Ile L-Isoleucine I
Leu L-Leucine L
Lys L-Lysine K
Met L-Methionine M
Phe L-Phenylalanine F
Pro L-Proline P
DPro D-Proline DP
Ser L-Serine S
Thr L-Threonine T
Trp L-Tryptophan W
Tyr L-Tyrosine Y
Val L-Valine V

Other Ξ±-amino acids which, or the residues of which, are suitable for the purposes of the present invention include:
Cit L-Citrulline
Orn L-Ornithine
tBuA L-t-Butylalanine
Sar Sarcosine
Pen L-Penicillamine
t-BuG L-tert-Butylglycine
4AmPhe L-para-Aminophenylalanine
3AmPhe L-meta-Aminophenylalanine
2AmPhe L-ortho-Aminophenylalanine
Phe(mC(NH2)═NH) L-meta-Amidinophenylalanine
Phe(pC(NH2)═NH) L-para-Amidinophenylalanine
Phe(mNHC(NH2)═NH) L-meta-Guanidinophenylalanine
Phe(pNHC(NH2)═NH) L-para-Guanidinophenylalanine
Phg L-Phenylglycine
Cha L-Cyclohexylalanine
C4al L-3-Cyclobutylalanine
C5al L-3-Cyclopentylalanine
Nle L-Norleucine
2-Nal L-2-Naphthylalanine
1-Nal L-1-Naphthylalanine
4Cl-Phe L-4-Chlorophenylalanine
3Cl-Phe L-3-Chlorophenylalanine
2Cl-Phe L-2-Chlorophenylalanine
3,4Cl2-Phe L-3,4-Dichlorophenylalanine
4F-Phe L-4-Fluorophenylalanine
3F-Phe L-3-Fluorophenylalanine
2F-Phe L-2-Fluorophenylalanine
Tic 1,2,3,4-Tetrahydroisoquinoline-3-
carboxylic acid
Thi L-Ξ²-2-Thienylalanine
Tza L-2-Thiazolylalanine
Mso L-Methionine sulfoxide
AcLys N-Acetyllysine
Dpr 2,3-Diaminopropionic acid
A2Bu 2,4-Diaminobutyric acid
Dbu (S)-2,3-Diaminobutyric acid
Abu Ξ³-Aminobutyric acid (GABA)
Aha Ξ΅-Aminohexanoic acid
Aib Ξ±-Aminoisobutyric acid
Y(Bzl) L-O-Benzyltyrosine
Bip L-(4-phenyl)phenylalanine
S(Bzl) L-O-Benzylserine
T(Bzl) L-O-Benzylthreonine
hCha L-Homo-cyclohexylalanine
hCys L-Homo-cysteine
hSer L-Homo-serine
hArg L-Homo-arginine
hPhe L-Homo-phenylalanine
Bpa L-4-Benzoylphenylalanine
4-AmPyrr1 (2S,4S)-4-Amino-pyrrolidine-L-carboxylic acid
4-AmPyrr2 (2S,4R)-4-Amino-pyrrolidine-L-carboxylic acid
4-PhePyrr1 (2S,5R)-4-Phenyl-pyrrolidine-L-carboxylic acid
4-PhePyrr2 (2S,5S)-4-Phenyl-pyrrolidine-L-carboxylic acid
5-PhePyrr1 (2S,5R)-5-Phenyl-pyrrolidine-L-carboxylic acid
5-PhePyrr2 (2S,5S)-5-Phenyl-pyrrolidine-L-carboxylic acid
Pro(4-OH)1 (4S)-L-Hydroxyproline
Pro(4-OH)2 (4R)-L-Hydroxyproline
Pip L-Pipecolic acid
DPip D-Pipecolic acid
OctG L-Octylglycine
MePhe L-N-Methylphenylalanine
MeNle L-N-Methylnorleucine
MeAla L-N-Methylalanine
MeIle L-N-Methylisoleucine
MeVal L-N-Methylvaline
MeLeu L-N-Methylleucine

Particularly preferred residues for group C are:
Ala L-Alanine
Ile L-Isoleucine
Leu L-Leucine
Met L-Methionine
Val L-Valine
tBuA L-t-Butylalanine
t-BuG L-tert-Butylglycine
Cha L-Cyclohexylalanine
C4al L-3-Cyclobutylalanine
C5al L-3-Cyclopentylalanine
Nle L-Norleucine
hCha L-Homo-cyclohexylalanine
OctG L-Octylglycine
MePhe L-N-Methylphenylalanine
MeNle L-N-Methylnorleucine
MeAla L-N-Methylalanine
MeIle L-N-Methylisoleucine
MeVal L-N-Methylvaline
MeLeu L-N-Methylleucine

Particularlily preferred residues for group D are:
His L-Histidine
Phe L-Phenylalanine
Trp L-Tryptophan
Tyr L-Tyrosine
Phg L-Phenylglycine
2-Nal L-2-Naphthylalanine
1-Nal L-1-Naphthylalanine
4Cl-Phe L-4-Chlorophenylalanine
3Cl-Phe L-3-Chlorophenylalanine
2Cl-Phe L-2-Chlorophenylalanine
3,4Cl2-Phe L-3,4-Dichlorophenylalanine
4F-Phe L-4-Fluorophenylalanine
3F-Phe L-3-Fluorophenylalanine
2F-Phe L-2-Fluorophenylalanine
Thi L-Ξ²-2-Thienylalanine
Tza L-2-Thiazolylalanine
Y(Bzl) L-O-Benzyltyrosine
Bip L-Biphenylalanine
S(Bzl) L-O-Benzylserine
T(Bzl) L-O-Benzylthreonine
hPhe L-Homo-phenylalanine
Bpa L-4-Benzoylphenylalanine

Particularly preferred residues for group E are
Arg L-Arginine
Lys L-Lysine
Orn L-Ornithine
Dpr L-2,3-Diaminopropionic acid
A2Bu L-2,4-Diaminobutyric acid
Dbu (S)-2,3-Diaminobutyric acid
Phe(pNH2) L-para-Aminophenylalanine
Phe(mNH2) L-meta-Aminophenylalanine
Phe(oNH2) L-ortho-Aminophenylalanine
hArg L-Homo-arginine
Phe(mC(NH2)═NH) L-meta-Amidinophenylalanine
Phe(pC(NH2)═NH) L-para-Amidinophenylalanine
Phe(mNHC(NH2)═NH) L-meta-Guanidinophenylalanine
Phe(pNHC(NH2)═NH) L-para-Guanidinophenylalanine
Cit L-Citrulline

Particularly preferred residues for group F are
Asn L-Asparagine
Cys L-Cysteine
Glu L-Glutamine
Ser L-Serine
Thr L-Threonine
Cit L-Citrulline
Pen L-Penicillamine
AcLys L-NΞ΅-Acetyllysine
hCys L-Homo-cysteine
hSer L-Homo-serine

In the dimeric structures Ib the preferred substituents forming groups G1 and G2 are the following, with the proviso that R33 is lower alkyl; or lower alkenyl; R34 is H; or lower alkyl; and R61 is H:

    • R2: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
    • R5: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R6: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R8: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R9: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R10: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R11: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
    • R14: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
    • R15: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
    • R16: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
    • R18: β€”(CH2)pOβ€”; β€”(CH2)pNR33R34β€”; β€”(CH2)pCOβ€”
    • R19: β€”(CH2)pOβ€”; β€”(CH2)pNR33R34β€”; β€”(CH2)pCOβ€”
    • R21: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R23: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R24: β€”(CH2)oOβ€”, β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R25: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
    • R26: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
    • R28: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R29: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)oCOβ€”
    • R31: β€”(CH2)pOβ€”; β€”(CH2)pNR33R34β€”; β€”(CH2)pCOβ€”
    • R37: β€”(CH2)pOβ€”; β€”(CH2)pNR33R34β€”; β€”(CH2)oCOβ€”
    • R38: β€”(CH2)pOβ€”; β€”(CH2)pNR33R34β€”; β€”(CH2)oCOβ€”
    • R41: β€”(CH2)pOβ€”; β€”(CH2)pNR33R34β€”; β€”(CH2)oCOβ€”
    • R42: β€”(CH2)pOβ€”; β€”(CH2)pNR33R34β€”; β€”(CH2)oCOβ€”
    • R45: β€”(CH2)oOβ€”; β€”(CH2)oNR33R34β€”; β€”(CH2)sCOβ€”
    • R47: β€”(CH2)oOβ€”
    • R49: β€”(CH2)sOβ€”; β€”(CH2)sCOβ€”
    • R51: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
    • R52: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
    • R53: β€”(CH2)mOβ€”; β€”(CH2)mNR33R34β€”; β€”(CH2)oCOβ€”
      and with the further provisos that the preferred linker molecules L are as defined below, that R34 is H; or lower alkyl; X is O; S; NR34; β€”NR34CONR34; or β€”OCOOβ€”; and Y is C6R67R68R69R70;
    • L1: β€”(CH2)p[X(CH2)p]oβ€”
    • L2: β€”CO(CH2)p[X(CHR2)p]oCOβ€”
    • L3: β€”CONR34(CH2)p[X(CH2)p]oNR34COβ€”
    • L4: β€”O(CH2)p[X(CH2)p]oOβ€”
    • L6: β€”NR34(CH2)p[X(CH2)p]oNR34β€”
    • L7: β€”(CH2)oY(CH2)oβ€”
    • L8: β€”CO(CH2)oY(CH2)oCOβ€”
    • L9: β€”CONR34(CH2)oY(CH2)oNR34COβ€”
    • L10: β€”O(CH2)oY(CH2)oOβ€”
    • L11:β€”S(CH2)oY(CH2)oSβ€”
    • L12: β€”NR34(CH2)oY(CH2)oNR34β€”
    • L13: β€”CO(CH2)p[X(CH2)p]oNR34β€”
    • L14: β€”CO(CH2)oY(CH2)oNR34β€”
    • L15 β€”NR34(CH2)p[X(CH2)p]oCOβ€”
    • L16 β€”NR34(CH2)oY(CH2)oCOβ€”
      with the proviso that
  • β€”(CH2)mOβ€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)oOβ€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)pOβ€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)sOβ€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)mNR34β€” can be combined with liker L, L2, L3, L7, L8 or L9;
  • β€”(CH2)oNR34β€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)pNR34β€” can be combined with linker L1, L2, L3, L7, L8 or L9;
  • β€”(CH2)oCOβ€” can be combined with linker L4, L5, L6, L10, L11 or L12;
  • β€”(CH2)pCOβ€” can be combined with linker L4, L5, L6, L10, L11 or L12;
  • β€”(CH2)sCOβ€” can be combined with linker L4, L5, L6, L10, L11 or L12;
  • β€”(CH2)mOβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)oCOβ€”; β€”(CH2)pCOβ€”; or β€”(CH2)sCOβ€”;
  • β€”(CH2)oOβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)oCOβ€”; β€”(CH2)pCOβ€”; or β€”(CH2)sCOβ€”;
  • (CH2)pOβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)oCOβ€”; β€”(CH2)pCOβ€”; or β€”(CH2)sCOβ€”;
  • β€”(CH2)sOβ€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)oCOβ€”; β€”(CH2)pCOβ€”; or β€”(CH2)sCOβ€”;
  • β€”(CH2)mNR34β€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)oCOβ€”; β€”(CH2)pCOβ€”; or β€”(CH2)sCOβ€”;
  • β€”(CH2)oNR34β€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)oCOβ€”; β€”(CH2)pCOβ€”; or β€”(CH2)sCOβ€”;
  • β€”(CH2)pNR34β€” can be combined with linker L13 or L14 and the resulting combination with β€”(CH2)oCOβ€”; β€”(CH2)pCOβ€”; or β€”(CH2)sCOβ€”;
  • β€”(CH2)oCOβ€” can be combined with linker L15 or L16 and the resulting combination with β€”(CH2)mXβ€”; β€”(CH2)oXβ€”; β€”(CH2)pXβ€”; or β€”(CH2)qβ€”;
  • β€”(CH2)pCOβ€” can be combined with linker L15 or L16 and the resulting combination with β€”(CH2)mXβ€”; β€”(CH2)oXβ€”; β€”(CH2)pXβ€”; or β€”(CH2)qXβ€”;
  • β€”(CH2)sCOβ€” can be combined with linker L15 or L16 and the resulting combination with β€”(CH2)mXβ€”; β€”(CH2)oXβ€”; β€”(CH2)pXβ€”; or β€”(CH2)qXβ€”.

Generally, the peptidic chain Z, Z1 or Z2 within the Ξ²-hairpin mimetics of the invention comprises 8–16 amino acid residues (n=8–16). The positions P1 to Pn of each amino acid residue in the chain Z, Z1 or Z2 are unequivocally defined as follows: P1 represents the first amino acid in the chain Z, Z1 or Z2 that is coupled with its N-terminus to the C-terminus of the templates (b)–(p) or of group β€”Bβ€”COβ€” in template (a1), or of group -A-COβ€” in template a2, and Pn represents the last amino acid in the chain Z, Z1 or Z2 that is coupled with its C-terminus to the N-terminus of the templates (b)–(p) or of group -A-COβ€” in template (a1) or of group β€”Bβ€”COβ€” in template (a2). Each of the positions P1 to Pn will preferably contain an amino acid residue belonging to one or two of above types C to F, as follows:

    • If n is 8, the amino acid residues in position 1–8 are preferably:
      • P1: of type C or of type D; or of type E;
      • P2: of type E; or of type D;
      • P3: of type E;
      • P4: of type E or of formula -A1–A69-COβ€”;
      • P5: of type E or of formula β€”Bβ€”COβ€”;
      • P6: of type D;
      • P7: of type E; or of type D and
      • P8: of type C or of type D; or of type E;
      • at P4 and P5 also D-isomers being possible;
    • if n is 9, the amino acid residues in position 1–9 are preferably:
      • P1: of type C or of type D; or of type E;
      • P2: of type E; or of type D;
      • P3: of type C;
      • P4: of type E, or the residue is Pro;
      • P5: of type E, or the residue is Pro;
      • P6: of type D or of type E, or the residue is Pro;
      • P7: of type E or of type D;
      • P8: of type E; or of type D and
      • P9: of type C or of type D; or of type E;
      • at P4, P5 and P6 also D isomers being possible;
    • if n is 10, the amino acid residues in position 1–10 are preferably:
      • P1: of type C or of type D; or of type E;
      • P2: of type E; or of type D;
      • P3: of type C;
      • P4: of type E or of type D;
      • P5: of type E or of formula -A1–A69COβ€”;
      • P6: of type E or of formula β€”Bβ€”COβ€”;
      • P7: of type D or of type E;
      • P8: of type D;
      • P9: of type E; or of type D and
      • P10: of type C or of type D; or of type E;
      • at P5 and P6 also D-isomers being possible;
    • if n is 11, the amino acid residues in position 1–11 are preferably:
      • P1: of type C or of type D; or of type E;
      • P2: of type E; or of type D;
      • P3: of type D;
      • P4: of type E or of type C;
      • P5: of type E, or the residue is Pro;
      • P6: of type E, or the residue is Pro;
      • P7: of type E, or the residue is Pro;
      • P8: of type D or of type E;
      • P9: of type D;
      • P10: of type E; or of type D and
      • P11: of type C or of type D; or of type E;
      • at P5, P6 and P7 also D-isomers being possible;
    • if n is 12, the amino acid residues in position 1–12 are preferably:
      • P1: of type C or of type E; or of type D; or of type F;
      • P2: of type E; or of type D;
      • P3: of type C or of type D;
      • P4: of type E;
      • P5: of type E; or of type C;
      • P6: of type E or of type F or of formula -A1–A69-COβ€”;
      • P7: of type E or of formula β€”Bβ€”COβ€”;
      • P8: of type D;
      • P9: of type E or of ype D;
      • P10: of type D;
      • P11: of type E; or of type D and
      • P12: of type C or of type E; or of type D; or of type F;
      • at P6 and P7 also D-isomers being possible;
    • if n is 13, the amino acid residues in position 1–13 are preferably:
      • P1: of type C or of type D; or of type E;
      • P2: of type E; or of type D;
      • P3: of type C or of type D;
      • P4: of type E or of type C;
      • P5: of type E or of type D;
      • P6: of type E or of type F, or the residue is Pro;
      • P7: of type E, or the residue is Pro;
      • P8: of type D, or the residue is Pro;
      • P9: of type D;
      • P10: of type E or of type C;
      • P11: of type C or of type D;
      • P12: of type E; or of type D and
      • P13: of type C or of type D; or of type E;
      • at P6, P7 and P8 also D-isomers being possible;
    • if n is 14, the amino acid residues in position 1–14 are preferably:
      • P1: of type C or of type D; or of type E;
      • P2: of type E; or of type D;
      • P3: of type C or of type D;
      • P4: of type D;
      • P5: of type E;
      • P6: of type E;
      • P7: of type E or of type F or of formula -A1–A69-COβ€”;
      • P8: of type E or of formula β€”Bβ€”COβ€”;
      • P9: of type D;
      • P10: of type C;
      • P11: of type E or of type D;
      • P12: of type D or of type C;
      • P13: of type E; or of type D and
      • P14: of type C or of type D; or of type E;
      • at P7 and P8 also D-isomers being possible;
    • if n is 15, the amino acid residues in position 1–15 are preferably:
      • P1: of type C and of type D; or of type E;
      • P2: of type E; or of type D;
      • P3: of type C and of type D;
      • P4: of type E or of type C;
      • P5: of type C;
      • P6: of type E or of type D;
      • P7: of type C, or the residue is Pro;
      • P8: of type E or of type F, or the residue is Pro;
      • P9: of type E or of type F, or the residue is Pro;
      • P10: of type E;
      • P11: of type C;
      • P12: of type E or of type C;
      • P13: of type D or of type C;
      • P14: of type E; or of type D and
      • P15: of type C and of type D; or of type E;
      • at P7, P8 and P9 also D-isomers being possible; and
    • if n is 16, the amino acid residues in position 1–16 are preferably:
      • P1: of type D; or of type E;
      • P2: of type E; or of type D;
      • P3: of type C or of type D;
      • P4: of type E or of type D;
      • P5: of type D;
      • P6: of type E;
      • P7: of type E or of type F;
      • P8: of type E or of type F or of formula -A1–A69-COβ€”;
      • P9: of type E or of formula β€”Bβ€”COβ€”;
      • P10: of type D;
      • P11: of type E;
      • P12: of type D;
      • P13: of type E or of type C;
      • P14: of type C or of type D;
      • P15: of type E; or of type D and
      • P16: of type C or of type D; or of type E;
      • at P8 and P9 also D-isomers being possible.

If n is 12, the amino acid residues in position 1–12 are most preferably:

    • P1: Leu; Arg; Lys; Tyr; Trp; Val; Gln; or 4-AmPhe;
    • P2: Arg; Trp; or Gln;
    • P3: Leu; Val; Ile; or Phe;
    • P4: Lys; Arg; Gln; or Orn;
    • P5: Lys; or Arg,
    • P6: Arg; Y(Bzl); or DY(Bzl);
    • P7: Arg;
    • P8: Trp; Bip; 1-Nal; Y(Bzl); or Val;
    • P9: Lys; Arg; Orn; Tyr, Trp; or Gln;
    • P10: Tyr; T(Bzl); or Y(Bzl);
    • P11: Arg; or Tyr; and
    • P12: Val; Arg; 1-Nal; or 4-AmPhe.

Particularly preferred Ξ²-peptidomimetics of the invention include those described in Examples 106, 137, 161, 197, 206, 222, 230, 250, 256, 267, 277, 281, 283, 284, 285, 286, 289, 294, 295, 296, 297, and 298.

The process of the invention can advantageously be carried out as parallel array synthesis to yield libraries of template-fixed Ξ²-hairpin peptidomimetics of the above general formula I. Such parallel synthesis allows one to obtain arrays of numerous (normally 24 to 192, typically 96) compounds of general formula I in high yields and defined purities, minimizing the formation of dimeric and polymeric by-products. The proper choice of the functionalized solid-support (i.e. solid support plus linker molecule), templates and site of cyclization play thereby key roles.

The functionalized solid support is conveniently derived from polystyrene crosslinked with, preferably 1–5%, divinylbenzene; polystyrene coated with polyethyleneglycol spacers (TentagelR); and polyacrylamide resins (see also Obrecht, D.; Villalgordo, J.-M, β€œSolid-Supported Combinatorial and Parallel Synthesis of Small-Molecular-Weight Compound Libraries”, Tetrahedron Organic Chemistry Series, Vol. 17, Pergamon, Elsevier Science, 1998).

The solid support is functionalized by means of a linker, i.e. a bifunctional spacer molecule which contains on one end an anchoring group for attachment to the solid support and on the other end a selectively cleavable functional group used for the subsequent chemical transformations and cleavage procedures. For the purposes of the present invention the linker must be designed to eventually release the carboxyl group under mild acidic conditions which do not affect protecting groups present on any functional group in the side-chains of the various amino acids. Linkers which are suitable for the purposes of the present invention form acid-labile esters with the carboxyl group of the amino acids, usually acid-labile benzyl, benzhydryl and trityl esters; examples of linker structures of this kind include 2-methoxy-4-hydroxymethylphenoxy (SasrinR linker), 4-(2,4-dimethoxyphenyl-hydroxymethyl)-phenoxy (Rink linker), 4-(4-hydroxymethyl-3-methoxyphenoxy)butyric acid (HMPB linker), trityl and 2-chlorotrityl.

Preferably, the support is derived from polystyrene crosslinked with, most preferably 1–5%, divinylbenzene and functionalized by means of the 2-chlorotrityl linker.

When carried out as a parallel array synthesis the process of the invention can be advantageously carried out as described hereinbelow but it will be immediately apparent to those skilled in the art how this procedure will have to be modified in case it is desired to synthesize one single compound of the above formula Ia or Ib.

A number of reaction vessels (normally 24 to 192, typically 96) equal to the total number of compounds to be synthesized by the parallel method are loaded with 25 to 1000 mg, preferably 100 mg, of the appropriate functionalized solid support, preferably 1 to 3% cross linked polystyrene or tentagel resin.

The solvent to be used must be capable of swelling the resin and includes, but is not limited to, dichloromethane (DCM), dimethylformamide (DMF), N-methylpyrrolidone (NMP), dioxane, toluene, tetrahydrofuran (THF), ethanol (EtOH), trifluoroethanol (TFE), isopropylalcohol and the like. Solvent mixtures containing as at least one component a polar solvent (e.g. 20% TFE/DCM, 35% THF/NMP) are beneficial for ensuring high reactivity and solvation of the resin-bound peptide chains (Fields, G. B., Fields, C. G., J. Am. Chem. Soc. 1991, 113, 4202–4207).

With the development of various linkers that release the C-terminal carboxylic acid group under mild acidic conditions, not affecting acid-labile groups protecting functional groups in the side chain(s), considerable progresses have been made in the synthesis of protected peptide fragments. The 2-methoxy-4-hydroxybenzylalcohol-derived linker (SasrinR linker, Mergler et al., Tetrahedron Lett. 1988, 29 4005–4008) is cleavable with diluted trifluoroacetic acid (0.5–1% TFA in DCM) and is stable to Fmoc deprotection conditions during the peptide synthesis, Boc/tBu-based additional protecting groups being compatible with this protection scheme. Other linkers which are suitable for the process of the invention include the super acid labile 4-(2,4-dimethoxyphenyl-hydroxymethyl)-phenoxy linker (Rink linker, Rink, H. Tetrahedron Lett. 1987, 28, 3787–3790), where the removal of the peptide requires 10% acetic acid in DCM or 0.2% trifluoroacetic acid in DCM; the 4-(4-hydroxymethyl-3-methoxyphenoxy)butyric acid-derived linker (HMPB-linker, Florsheimer & Riniker, Peptides 1991, 1990 131) which is also cleaved with 1% TFA/DCM in order to yield a peptide fragment containing all acid labile side-chain protective groups; and, in addition, the 2-chlorotritylchloride linker (Barlos et al., Tetrahedron Lett. 1989, 30, 3943–3946), which allows the peptide detachment using a mixture of glacial acetic acid/trifluoroethanol/DCM (1:2:7) for 30 min.

Suitable protecting groups for amino acids and, respectively, for their residues are, for example,

    • for the amino group (as is present e. g. also in the side-chain of lysine)
Cbz benzyloxycarbonyl
Boc tert.-butyloxycarbonyl
Fmoc 9-fluorenylmethoxycarbonyl
Alloc allyloxycarbonyl
Teoc trimethylsilylethoxycarbonyl
Tcc trichloroethoxycarbonyl
Nps o-nitrophenylsulfonyl;
Trt triphenymethyl or trityl

    • for the carboxyl group (as is present e. g. also in the side-chain of aspartic and glutamic acid) by conversion into esters with the alcohol components
tBu tert.-butyl
Bn benzyl
Me methyl
Ph phenyl
Pac Phenacyl
Allyl
Tse trimethylsilylethyl
Tce trichloroethyl;

    • for the guanidino group (as is present e. g. in the side-chain of arginine)
Pmc 2,2,5,7,8-pentamethylchroman-6-sulfonyl
Ts tosyl (i.e. p-toluenesulfonyl)
Cbz benzyloxycarbonyl
Pbf pentamethyldihydrobenzofuran-5-sulfonyl

    • for the hydroxy group (as is present e. g. in the side-chain of threonine and serine)
tBu tert.-butyl
Bn benzyl
Trt trityl

    • and for the mercapto group (as is present e. g. in the side-chain of cysteine)
Acm acetamidomethyl
tBu tert.-butyl
Bn benzyl
Trt trityl
Mtr 4-methoxytrityl.

The 9-fluorenylmethoxycarbonyl-(Fmoc)-protected amino acid derivatives are preferably used as the building blocks for the construction of the template-fixed Ξ²-hairpin loop mimetics of formulae Ia and Ib. For the deprotection, i.e. cleaving off of the Fmoc group, 20% piperidine in DMF or 2% DBU/2% piperidine in DMF can be used.

The quantity of the reactant, i.e. of the amino acid derivative, is usually 1 to 20 equivalents based on the milliequivalents per gram (meq/g) loading of the functionalized solid support (typically 0.1 to 2.85 meq/g for polystyrene resins) originally weighed into the reaction tube. Additional equivalents of reactants can be used if required to drive the reaction to completion in a reasonable time. The reaction tubes, in combination with the holder block and the manifold, are reinserted into the reservoir block and the apparatus is fastened together. Gas flow through the manifold is initiated to provide a controlled environment, for example, nitrogen, argon, air and the like. The gas flow may also be heated or chilled prior to flow through the manifold. Heating or cooling of the reaction wells is achieved by heating the reaction block or cooling externally with isopropanol/dry ice and the like to bring about the desired synthetic reactions. Agitation is achieved by shaking or magnetic stirring (within the reaction tube). The preferred workstations (without, however, being limited thereto) are Labsource's Combi-chem station and MultiSyn Tech's-Syro synthesizer.

Amide bond formation requires the activation of the Ξ±-carboxyl group for the acylation step. When this activation is being carried out by means of the commonly used carbodiimides such as dicyclohexylcarbodiimide (DCC, Sheehan & Hess, J. Am. Chem. Soc. 1955, 77, 1067–1068) or diisopropylcarbodiimidc (DIC, Sarantakis et al Biochem Biophys. Res. Commun. 1976, 73, 336–342), the resulting dicyclohexylurea is insoluble and, respectively, diisopropylurea is soluble in the solvents generally used. In a variation of the carbodiimide method 1-hydroxybenzotriazole (HOBt, KΓΆnig & Geiger, Chem. Ber 1970, 103, 788–798) is included as an additive to the coupling mixture. HOBt prevents dehydration, suppresses racemization of the activated amino acids and acts as a catalyst to improve the sluggish coupling reactions. Certain phosphonium reagents have been used as direct coupling reagents, such as benzotriazol-1-yl-oxy-tris-(dimethylamino)-phosphonium hexafluorophosphate (BOP) (Castro et al., Tetrahedron Lett. 1975, 14, 1219–1222; Synthesis, 1976, 751–752), or benzotriazol-1-yl-oxy-tris-pyrrolidino-phosphonium hexaflurophoshate (Py-BOP, Coste et al., Tetrahedron Lett. 1990, 31, 205–208), or 2-(1H-benzotriazol-1-yl-)1,1,3,3-tetramethyluronium terafluoroborate (TBTU), or hexafluorophosphate (HBTU, Knorr et al., Tetrahedron Lett. 1989, 30, 1927–1930); these phosphonium reagents are also suitable for in situ formation of HOBt esters with the protected amino acid derivatives. More recently diphenoxyphosphoryl azide (DPPA) or O-(7-aza-benzotriazol-1-yl)-N,N,Nβ€²,Nβ€²-tetramethyluronium tetrafluoroborate (TATU) or O-(7-aza-benzotriazol-1-yl)-N,N,Nβ€²,Nβ€²-tetramethyluronium hexafluorophosphate (HATU)/7-aza-1-hydroxy benzotriazole (HOAt, Carpino et al., Tetrahedron Lett. 1994, 35, 2279–2281) have also been used as coupling reagents.

Due to the fact that near-quantitative coupling reactions are essential it is desirable to have experimental evidence for completion of the reactions. The ninhydrin test raiser et al., Anal. Biochemistry 1970, 34, 595), where a positive colorimetric response to an aliquot of resin-bound peptide indicates qualitatively the presence of the primary amine, can easily and quickly be performed after each coupling step. Fmoc chemistry allows the spectrophotometric detection of the Fmoc chromophore when it is released with the base (Meienhofer et al., Int. J. Peptide Protein Res. 1979, 13, 35–42).

The resin-bound intermediate within each reaction tube is washed free of excess of retained reagents, of solvents, and of by-products by repetitive exposure to pure solvent(s) by one of the two following methods:

  • 1) The reaction wells are filled with solvent (preferably 5 ml), the reaction tubes, in combination with the holder block and manifold, are immersed and agitated for 5 to 300 minutes, preferably 15 minutes, and drained by gravity followed by gas pressure applied through the manifold inlet (while closing the outlet) to expel the solvent;
  • 2) The manifold is removed from the holder block, aliquots of solvent (preferably 5 ml) are dispensed through the top of the reaction tubes and drained by gravity through a filter into a receiving vessel such as a test tube or vial.

Both of the above washing procedures are repeated up to about 50 times (preferably about 10 times), monitoring the efficiency of reagent, solvent, and byproduct removal by methods such as TLC, GC, or inspection of the washings.

The above described procedure of reacting the resin-bound compound with reagents within the reaction wells followed by removal of excess reagents, by-products, and solvents is repeated with each successive transformation until the final Tesin-bound fully protected linear peptide has been obtained.

Before this fully protected linear peptide is detached from the solid support, it is possible, if desired, to selectively deprotect one or several protected functional group(s) present in the molecule and to appropriately substitute the reactive group(s) thus liberated. To this effect, the functional group(s) in question must initially be protected by a protecting group which can be selectively removed without affecting the remaining protecting groups present. Alloc (alkyloxycarbonyl) is an example for such a protecting group for amino which can be selectively removed, e.g. by means of PdΒ° and phenylsilane in CH2Cl2, without affecting the remaining protecting groups, such as Fmoc, present in the molecule. The reactive group thus liberated can then be treated with an agent suitable for introducing the desired substituent. Thus, for example, an amino group can be acylated by means of an acylating agent corresponding to the acyl substituent to be introduced.

Detachment of the fully protected linear peptide from the solid support is achieved by immersion of the reaction tubes, in combination with the holder block and manifold, in reaction wells containing a solution of the cleavage reagent (preferably 3 to 5 ml). Gas flow, temperature control, agitation, and reaction monitoring are implemented as described above and as desired to effect the detachment reaction. The reaction tubes, in combination with the holder block and manifold, are disassembled from the reservoir block and raised above the solution level but below the upper lip of the reaction wells, and gas pressure is applied through the manifold inlet (while closing the outlet) to efficiently expel the final product solution into the reservoir wells. The resin remaining in the reaction tubes is then washed 2 to 5 times as above with 3 to 5 ml of an appropriate solvent to extract (wash out) as much of the detached product as possible. The product solutions thus obtained are combined, taking care to avoid cross-mixing. The individual solutions/extracts are then manipulated as needed to isolate the final compounds. Typical manipulations include, but are not limited to, evaporation, concentration, liquid/liquid extraction, acidification, basification, neutralization or additional reactions in solution.

The solutions containing fully protected linear peptide derivatives which have been cleaved off from the solid support and neutralized with a base, are evaporated. Cyclization is then effected in solution using solvents such as DCM, DMF, dioxane, ThF and the like. Various coupling reagents which were mentioned earlier can be used for the cyclization. The duration of the cyclization is about 6–48 hours, preferably about 24 hours. The progress of the reaction is followed, e.g. by RP-HPLC (Reverse Phase High Performance Liquid Chromatography). Then the solvent is removed by evaporation, the fully protected cyclic peptide derivative is dissolved in a solvent which is not miscible with water, such as DCM, and the solution is extracted with water or a mixture of water-miscible solvents, in order to remove any excess of the coupling reagent.

Before removing the protecting groups from the fully protected cyclic peptide, it is possible, if desired, to form an interstrand linkage between side-chains of appropriate amino acid residues at opposite positions of the Ξ²-strand region; and/or to connect two building blocks of the type of formula Ia via a bridge -G1-L-G2- to give a dimeric structure of the type of formula Ib.

Interstrand linkages and their formation have been discussed above, in connection with the explanations made regarding groups of the type H which can, for example, be disulfide bridges formed by cysteines and homocysteines at opposite positions of the Ξ²-strand, or glutamic and aspartic acid residues linking ornithines and, respectively, lysines located at opposite Ξ²-strand positions by amide bond formation. The formation of such interstrand linkages can be effected by methods well known in the art.

Interstrand linkages and their formation have been discussed above, in connection with the explanations made regarding groups of the type H which can, for example, be disulfide bridges formed by cysteines and homocysteines at opposite positions of the Ξ²-strand, or glutamic and aspartic acid residues linking ornithines and, respectively, lysines located at opposite Ξ²-strand positions by amide bond formation. The formation of such interstrand linkages can be effected by methods well known in the art.

For building up a bridge -G1-L-G2- to give a dimeric structure, methods well known in the art can be used, too. Thus, for example, a fully side-chain protected Ξ²-hairpin peptidomimetic carrying a group G1 or G2 containing an appropriately protected alcohol group (e.g. as tert.-butyldiphenylsilyl protected), thiol group (e.g. as acetamidomethyl protected) or amino group (NR34; e.g. as alkyloxycarbonyl protected) can selectively be deprotected employing methods well known by the skilled in the art and reacted with suitably activated linker (L) precursors; e.g:

    • for L1 the corresponding building block is Br(Cl,I)(CH2)pCHR61[X(CH2)pCHR61]oOH: the resulting alcohol can be transformed into the corresponding bromide (chloride or iodide) by methods well known to those skilled in the art (e.g. P(Ph)3, CBr4) and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing an alcohol, thiol or amine group. The dimeric fully side-chain protected molecule can be fully deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • for L2 the corresponding building block is ClOC(CH2)pCHR61[X(CH2)pCHR61]oCOOAllyl: the resulting ester can be transformed into the corresponding acid by methods well known in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing an alcohol, thiol or amine group. The dimeric fully side-chain protected molecule can be fully deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L3 the corresponding building block is O═C═N(CH2)pCHR61[X(CH2)pCHR61]oNR34Alloc: the resulting Alloc-protected amine can be deprotected and transformed into the corresponding isocyanate by methods familiar to those skilled in the art (e.g. triphosgene) and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing an alcohol, thiol or amine group. The dimeric fully side-chain protected molecule can be fully deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L7 the corresponding building block is Br(Cl,I)(CH2)oCHR61Y(CH2)oCHR61OH: the resulting alcohol can be transformed into the corresponding bromide (chloride or iodide) by methods well known in the art (e.g. P(Ph)3, CBr4) and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing an alcohol, thiol or amine group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L8 the corresponding building block is ClOC(CH2)oCHR61Y(CH2)oCHR61COOAllyl: the resulting ester can be transformed into the corresponding acid by methods well known to those skilled in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing an alcohol, thiol or amine group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L9 the corresponding building block is O═C═N(CH2)oCHR61Y(CH2)oCHR61NR34Alloc: the resulting Alloc-protected amine can be deprotected and transformed into the corresponding isocyanate by methods well known in the art (e.g. triphosgene) and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing an alcohol, thiol or amine group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L13 the corresponding building block is ClOC(CH2)pCHR61[X(CH2)pCHR61]oNR34Alloc: the resulting Alloc-protected amine can be deprotected by methods readily available to those skilled in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing a carboxylic acid group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L14 the corresponding building block is ClOC(CH2)oCHR61Y(CH2)oCHR61N34Alloc: the resulting Alloc-protected amine can be deprotected by conventional methods and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing a carboxylic acid group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.

Alternatively, a fully side-chain protected Ξ²-hairpin peptidomimetic carrying a group G1 or G2 containing an appropriately protected thiol group (e.g. as acetamidomethyl protected) can selectively be deprotected employing methods well known to those skilled in the art and reacted with a second Ξ²-hairpin peptidomimetic carrying a group G1 or G2 containing a thiol group forming a disulfide bond by oxidation (air or iodine). The dimeric molecule can subsequently be fully deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.

Finally, a fully side-chain protected Ξ²-hairpin peptidomimetic carrying a group G1 or G2 containing an appropriately protected carboxylic acid group (e.g. alkyl ester), can selectively be deprotected employing methods well known in the art and reacted with a suitably activated linker (L) precursor; e.g:

    • For L4 the corresponding building block is HO(CH2)pCHR61[X(CH2)pCHR61]oOAlloc: the resulting Alloc-protected alcohol can be deprotected by methods well known to those skilled in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing a carboxylic acid group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L5 the corresponding building block is HS(CH2)pCHR61[X(CH2)pCHR61]oSAlloc: the resulting Alloc-protected thiol can be deprotected by methods well known in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing a carboxylic acid group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L6 the corresponding building block is HNR34(CH2)pCHR61[X(CH2)pCHR61]oNR34Alloc: the resulting Alloc-protected amine can be deprotected by methods familiar to those skilled in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing a carboxylic acid group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L10 the corresponding building block is HO(CH2)oCHR61Y(CH2)CHR61OAlloc: the resulting Alloc-protected alcohol can be deprotected by methods well known to those skilled in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing a carboxylic acid group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L11 the corresponding building block is HS(CH2)oCHR61Y(CH2)oCHR61SAlloc: the resulting Alloc-protected thiol can be deprotected by methods well known in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing a carboxylic acid group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L12 the corresponding building block is HNR34(CH2)oCHR61Y(CH2)oCHR61NR34Alloc: the resulting Alloc-protected amine can be deprotected by methods well known to those skilled in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing a carboxylic acid group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L15 the corresponding building block is HNR34(CH2)pCHR61[X(CH2)pCHR61]oCOOAllyl: the resulting Allylester can be deprotected by conventional methods and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing an alcohol group, a thiol group or an amino (NR34) group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.
    • For L16 the corresponding building block is HNR34(CH2)oCHR61Y(CH2)oCHR61COOAllyl: the resulting Allylester can be deprotected by methods well known to those skilled in the art and combined with a second Ξ²-hairpin mimetic carrying a group G1 or G2 containing an alcohol group, a thiol group or an amino (NR34) group. The dimeric fully side-chain protected molecule can be deprotected and purified by preparative HPLC chromatography as described in procedure 1, hereinbelow.

Finally, the fully protected peptide derivative of type Ia or Ib is treated with 95% TFA, 2.5% H2O, 2.5% TIS or another combination of scavengers for effecting the cleavage of protecting groups. The cleavage reaction time is commonly 30 minutes to 12 hours, preferably about 2 hours. Thereafter most of the TFA is evaporated and the product is precipitated with ether/hexane (1:1) or other solvents which are suitable therefor. After careful removal of the solvent, the cyclic peptide derivative obtained as end-product can be isolated. Depending on its purity, this peptide derivative can be used directly for biological assays, or it has to be further purified, for example by preparative HPLC.

As mentioned earlier, it is thereafter possible, if desired, to convert a fully deprotected product thus obtained into a pharmaceutically acceptable salt or to convert a pharmaceutically acceptable, or unacceptable, salt thus obtained into the corresponding free compound of formula Ia and Ib or into a different, pharmaceutically acceptable, salt. Any of these operations can be carried out by methods well known in the art.

The starting materials used in the process of the invention, pre-starting materials therefor, and the preparation of these starting and pre-starting materials will now be discussed in detail.

Building blocks of type A can be synthesized according to the literature methods described below. The corresponding amino acids have been described either as unprotected or as Boc- or Fmoc-protected racemates, (D) or (L)-isomers. It will be appreciated that unprotected amino acid building blocks can be easily transformed into the corresponding Fmoc-protected amino acid building blocks required for the present invention by standard protecting group manipulations. Reviews describing general methods for the synthesis of Ξ±-amino acids include: R. Duthaler, Tetrahedron (Report) 1994, 349, 1540–1650; R. M. Williams, β€œSynthesis of optically active Ξ±-amino acids”, Tetrahedron Organic Chemistry Series, Vol. 7, J. E. Baldwin, P. D. Magnus (Eds.), Pergamon Press., Oxford 1989. An especially useful method for the synthesis of optically active Ξ±-amino acids relevant for this invention includes kinetic resolution using hydrolytic enzymes (M. A. Verhovskaya, I. A. Yamskov, Russian Chem. Rev. 1991, 60, 1163–1179; R. M. Williams, β€œSynthesis of optically active Ξ±-amino acids”, Tetrahedron Organic Chemistry Series, Vol. 7, J. E. Baldwin, P. D. Magnus (Eds.), Pergamon Press., Oxford 1989, Chapter 7, p. 257–279). Hydrolytic enzymes involve hydrolysis of amides and nitrites by aminopeptidases or nitrilases, cleavage of N-acyl groups by acylases, and ester hydrolysis by lipases or proteases. It is well documented that certain enzymes will lead specifically to pure (L)-enantiomers whereas others yield the corresponding (D)-enantiomers (e.g.: R. Duthaler, Tetrahedron Report 1994, 349, 1540–1650; R. M. Williams, β€œSynthesis of optically active Ξ±-amino acids”, Tetrahedron Organic Chemistry Series, Vol. 7, J. E. Baldwin, P. D. Magnus (Eds.), Pergamon Press., Oxford 1989).

A1: See D. Ben-Ishai, Tetrahedron 1977, 33, 881–883; K. Sato, A. P. Kozikowski, Tetrahedron Lett. 1989, 30, 4073–4076; J. E. Baldwin, C. N. Farthing, A. T. Russell, C. J. Schofield, A. C. Spirey, Tetrahedron Lett. 1996, 37, 3761–3767; J. E. Baldwin, R. M. Adlington, N. G. Robinson, J. Chem. Soc. Chem. Commun. 1987, 153–157; P. Wipf, Y. Uto, Tetrahedron Lett. 1999, 40, 5165–5170; J. E. Baldwin, R. M. Adlington, A. O'Neil, A. C. Spirey, J. B. Sweeney, J. Chem. Soc. Chem. Commun. 1989, 1852–1854 (for R1═H, R2═H); T. Hiyama, Bull. Chem. Soc. Jpn. 1974, 47, 2909–2910; T. Wakamiya, K. Shimbo, T. Shiba, K. Nakajima, M. Neya, K. Okawa, Bull. Chem. Soc. Jpn. 1982, 55, 3878–3881; I. Shima, N. Shimazaki, K. Imai, K. Hemmi, M. Hashimoto, Chem. Pharm. Bull. 1990, 38, 564–566; H. Han, J. Yoon, K. D. Janda, J. Org. Chem. 1998, 63, 2045–2048 (R1═H, R2=Me); J. Legters, G. H. Willems, L. Thijs, B. Zwannenburg, Recl. Trav. Chim. Pays-Bas 1992, 111, 59–68 (R1═H, R2=hexyl); J. Legters, L. Thijs, B. Zwannenburg, Recl. Trav. Chim. Pays-Bas 1992, 111, 16–21; G. A. Molander, P. J. Stengel, J. Org. Chem. 1995, 21, 6660–6661 (R1═H, R2=Ph); I. Funaki, L. Thijs, B. Zwannenburg, Tetrahedron 1996, 52, 9909–9924 (R1═H, R2=Bn); A. S. Pepito, D. C. Dittmer, J. Org. Chem. 1997, 62, 7920–7925; (R1═H, R2═CH2OH); M. Egli, A. S. Dreiding, Helv. Chim. Acta 1986, 69, 1442–1460 (R2═CH(OH)CH2OH); M. Carduccu, S. Fioravanti, M. A. Loreto, L. Pellacani, P. A. Tardella, Tetrahedron Lett. 1996, 37, 3777–3778; F. J. Lakner, L. P. Hager, Tetrahedron: Asymmetry 1997, 21, 3547–3550 (R1=Me, R2═H, Me); G. A. Molander, P. J. Stengel, Tetrahedron 1997, 26, 8887–8912; M. A. Loreto, F. Pompei, P. A. Tardella, D. Tofani, Tetrahedron 1997, 53, 15853–15858 (R1=Me, R2═CH2SiMe3); H. Shao, J. K. Rueter, M. Goodman, J. Org. Chem. 1998, 63, 5240–5244 (R1=Me, R2=Me).

A2: See A. Rao, M. K. GurjΓ€r, V. Vivarr, Tetrahedron: Asymmetry 1992, 3, 859–862; R. L. Johnson, G. Rayakumar, K.-L. Yu, R. K. Misra, J. Med. Chem. 1986, 29, 2104–2107 (R1═H, R2═H); J. E. Baldwin, R. M. Adlington, R. H. Jones, C. J. Schofield, C. Zarcostas, J. Chem. Soc. Chem. Commun. 1985, 196–196; J. E. Baldwin, R. M. Adlington, R. H. Jones, C. J. Schofield, C. Zarcostas, Tetrahedron 1986, 42, 4879–4888 (R1═H, R2═CH2OH, CH2CHO, CH2CH2COOH, CH2CH2OH); A. P. Kozikowski, W. Tueckmantel, I. J. Reynolds, J. T. Wroblewski, J. Med. Chem. 1990, 33, 1561–1571; A. P. Kozikowski, W. Tueclanantel, Y. Liao, H. Manev, S. Ikonomovic J. T. Wroblenski, J. Med. Chem. 1993, 36, 2706–2708 (R1═H, R2═CH2OH, CHCONH2, CONHCH2COOH, COOtBu); D. Seebach, T. Vettiger, H.-M. MΓΌller, D. Plattner, W. Petter, Liebigs Ann. Chem. 1990, 687–695 (R1═ArylCH(OH), R2═H); D. Seebach, E. Dziadulewicz, L. Behrendt, S. Cantoreggi, R. Fitzi, Liebigs Ann. Chem. 1989, 1215–1232 (R1=Me, Et, R2═H).

A3: See A. P. Kozikowski, Y. Liao, W. Tueckmantel, S. Wang, S. Pshsenichkin, Bioorg. Med. Chem. Lett. 1996, 6, 2559–2564 (R1═H; R2═CHCHO, CH2OH, CH2CH2OH, CH2COOH, COOH); Isono, J. Am. Chem. Soc, 1969, 91, 7490 (R1═H; R2=Et); P. J. Blythin, M. J. Green, M. J. Mary, H. Shue, J. Org. Chem. 1994, 59, 6098–6100; S. Hanessian, N. Bernstein, R.-Y. Yang, R. Maquire, Bioorg. Chem. Lett. 1994, 9, 1437–1442 (R1═H; R2=Ph).

A4: See G. Emmer, Tetrahedron 1992, 48, 7165–7172; M. P. Meyer, P. L. Feldman, H. Rapoport, J. Org. Chem. 1985, 50, 5223–5230 (R1═H; R2═H); A. J. Bose, M. S. Manhas, J. E. Vincent, I. F. Fernandez, J. Org. Chem. 1982, 47, 4075–4081 (R1═H; R2═NHCOCH2OPh); D. L. Boger, J. B. Meyers, J. Org. Chem. 1991, 56, 5385–5390 (R1═H; R2═NHCOCH2Ph); K.-D. Kampe, Tetrahedron Lett. 1969, 117–120 (R1═CH2OH; R2=Ph); M. D. Andrews, M. G. Maloney, K. L. Owen, J. Chem. Soc. Perkin Trans. 1, 1996, 227–228 (R1═CH2OH; R2═H).

A5: See C. Bisang, C. Weber, J. Inglis, C. A. Schiffer, W. F. van Gunsteren, J. A. Robinson J. Am. Chem. Soc. 1995, 117, 7904 (R1═CH3; R2═H); S. Takano, M. Morija, Y. Iwabuki, K. Ogasawara, Tetrahedron Lett. 1989, 30, 3805–3806 (R1═H; R2═COOH); M. D. Bachi, R. Breiman, H. Meshulam, J. Org. Chem. 1983, 48, 1439–1444 (R1═H; R2═CH(Et)COOH); D. S. Kemp, T. P. Curran, Tetrahedron Lett. 1988, 29, 4931–4934; D. S. Kemp, T. P. Curran, W. M. Davies, J. Org. Chem. 1991, 56, 6672–6682 (R1═H; R2═CH2OH); F. Manfre, J.-M. Kern, J.-F. Biellmann, J. Org. Chem. 1992, 57, 2060–2065 (R1═H; R2═H, CH═CH2, CCH); B. W. Bycroft, S. R. Chabra, J. Chem. Soc. Chem. Commun. 1989, 423–425 (R1═H; R2═CH2COOtBu; Y. Xu, J. Choi, M. I. Calaza, S. Turner, H. Rapoport, J. Org. Chem. 1999, 64, 4069–4078 (R1═H; R2=3-pyridyl); E. M. Khalil, W. J. Ojala, A. Pradham, V. D. Nair, W. B. Gleason, J. Med. Chem. 1999, 42, 628–637; E. M. Khalil, N. L. Subasinghe, R. L. Johnson, Tetrahedron Lett. 1996, 37, 3441–3444 (R1=alkyl; R2═H); A. DeNicola, J.-L. Luche, Tetrahedron Lett. 1992, 33, 6461–6464; S. Thaisrivongs, D. T. Pals, J. A. Lawson, S. Turner, D. W. Harris, J. Med. Chem. 1987, 30, 536–541; E. M. Khalil, N. L. Subasinghe, R. L. Johnson, Tetrahedron Lett. 1996, 37, 3441–3444; A. Lewis, J. Wilkie, T. J. Rutherford, D. Gani, J. Chem. Soc. Perkin Trans. 1, 1998, 3777–3794 (R1=Me; R2═H); A. Lewis, J. Wilkie, T. J. Rutherford, D. Gani, J. Chem. Soc. Perkin Trans. 1, 1998, 3777–3794 (R1═CH2COOMe; R2═H); N. L. Subasinghe, E. M. Khalil, R. L. Johnson, Tetrahedron Lett. 1997, 38, 1317–1320 (R1═CH2CHO; R2═H); D. J. Witter, S. J. Famiglietti, J. C. Gambier, A. L. Castelhano, Bioorg. Med. Chem. Lett. 1998, 8, 3137–3142; E. H. Khalil, W. H. Ojada, A. Pradham, V. D. Nair, W. B. Gleason, J. Med. Chem. 1999, 42, 628–637 (R1═CH2CH2CHO; R2═H).

A6: See DeNardo, Farmaco Ed. Sci. 1977, 32, 522–529 (R1═H; R3═H); P. J. T. Floris, N. Terhuis, H. Hiemstra, N. W. Speckamp, Tetrahedron, 1993, 49, 8605–8628; S. Kanemasa, N. Tomoshige, O. Tsuge, Bull. Chem. Soc. Jpn. 1989, 62, 3944–3949 (R1═H; R3═H); Sucrow, Chem. Ber. 1979, 112, 1719.

A7: See Fichter, J. Prakt. Chem. 1906, 74, 310 (R1=Me; R4=Ph).

A8: See L. Lapantsanis, G. Milias, K. Froussios, M. Kolovos, Synthesis 1983, 641–673; H. Nedev, H. Naharisoa, Tetrahedron Lett. 1993, 34, 4201–4204; D. Y. Jackson, C. Quan, D. R. Artis, T. Rawson, B. Blackburn, J. Med. Chem. 1997, 40, 3359–3368; D. Konopinska, H. Bartosz-Bechowski, G. Rosinski, W. Sobotka, Bull. Pol. Acad. Sci. Chem. 1993, 41, 27–40; J. Hondrelis, G. Lonergan, S. Voliotis, J. Matsukas, Tetrahedron 1990, 46, 565–576; T. Nakamura, H. Matsuyama, H. Kanigata, M. Iyoda, J. Org. Chem. 1992, 57, 3783–3789; C. E. O'Connell, K. Ackermanr, C. A. Rowell, A. Garcia, M. D. Lewis, C. E. Schwartz, Bioorg. Med. Chem. Lett. 1999, 9, 2095–2100; G. Lowe, T. Vilaivan, J. Chem. Soc. Perkin Trans. 1997, 547–554; B. Bellier, I. McCourt-Tranchepain, B. Ducos, S. Danascimenta, H. Mundal, J. Med. Chem. 1997, 40, 3947–3956; M. Peterson, R. Vince J. Med. Chem. 1991, 34, 2787–2797; E. M. Smith, G. F. Swiss, B. R. Neustadt, E. H. Gold, J. A. Sommer, J. Med. Chem. 1988, 31, 875–885; E. Rubini, C. Gilon, Z. Selinger, M. Chorev, Tetrahedron 1986, 42, 6039–6045 (R1═H; R5═OH); C. R. Noe, M. Knollmueller, H. Voellenkle, M. Noe-Letschnig, A. Weigand, J. MΓΌlh, Pharmazie, 1996, 51, 800–804 (R1═CH3; R5═OH); J. Kitchin, R. C. Berthel, N. Cammack, S. Dolan, D. N. Evans, J. Med. Chem. 1994, 37, 3703–3716; D. Y. Jackson, C. Quan, D. R. Artis, T. Rawson, B. Blackburn, J. Med. Chem. 1997, 40, 3359–3368 (R1═H; R5═OBn); J. E. Baldwin, A. R. Field, C. C. Lawrence, K. D. Merritt, C. J. Schofield, Tetrahedron Lett. 1993, 34, 7489–7492; K. Hashimoto, Y. Shima, H. Shirahama, Heterocycles 1996, 42, 489–492 (R1═H; R5═OTs); T. R. Webb, C. Eigenbrot, J. Org. Chem. 1991, 56, 3009–3016; D. C. Cafferty, C. A. Slate, B. M. Nakhle, H. D. Graham, T. L. Anstell, Tetrahedron 1995, 51, 9859–9872 (R1═H; R5═NH2); T. R. Webb, C. Eigenbrot, J. Org. Chem. 1991, 56, 3009–3016 (R1═H; R5═CH2NH2); J. K. Thottathil, J. L. Moniot, Tetrahedron Lett. 1986, 27, 151–154 (R1═H; R5=Ph); K. Plucinska, T. Kataoka, M. Yodo, W. Cody, J. Med. Chem. 1993, 36, 1902–1913 (R1═H; R5═SBn); J. Krapcho, C. Turk, D. W. Cushman, J. R. Powell, J. Med. Chem. 1988, 31, 1148–1160 (R1═H; R5═SPh); A. J. Verbiscar, B. Witkop, J. Org. Chem. 1970, 35, 1924–1927 (R1═H; R5═SCH2(4-OMe)C6H4); S. I. Klein, J. M. Denner, B. F. Molino, C. Gardner, R. D'Alisa, Bioorg. Med. Chem. Lett. 1996, 6, 2225–2230 (R1═H; R5═O(CH2)3Ph); R. Zhang, F. Brownewell, J. S. Madalengoita, Tetrahedron Lett. 1999, 40, 2707–2710 (R1═H; R5═CH2COOBn).

A9: See Blake, J. Am. Chem. Soc. 1964, 86, 5293–5297; J. Cooper, R. T. Gallagher, D. T. Knight, J. Chem. Soc. Chem. Perkin Trans. 1, 1993, 1313–1318; D. W. Knight, A. W. Sibley, J. Chem. Soc. Perkin Trans. 1, 1997, 2179, 2188 (R1═H; R6═H); Blake, J. Am. Chem. Soc. 1964, 86, 5293–5297; Y. Yamada, T. Ishii, M. Kimura, K. Hosaka, Tetrahedron Lett. 1981, 1353–1354 (R1═H; R6═OH); Y. Umio, Yakugahu Zasshi, 1958, 78, 727 (R1═H; R6=iPr); Miyamoto, Yahugaku Zasshi, 1957, 77, 580–584; Tanaka, Proc. Jpn. Acad. 1957, 33, 47–50 (R1═H; R6═CH(CH3)CH2N(CH3)2); L. E. Overman, B. N. Rodgers, J. E. Tellew, W. C. Trenkle, J. Am. Chem. Soc. 1997, 119, 7159–7160 (R1═H; R6=alkyl); Ohki, Chem. Pharm. Bull. 1976, 24, 1362–1369 (R1═CH3; R6═H).

A10: See J. Mulzer, A. Meier, J. Buschmann, P. Luger, Synthesis 1996, 123–132 (R1═H; R7═CH═CH2); J. Cooper, P. T. Gallagher, D. W. Knight, J. Chem. Soc. Chem. Commun. 1988, 509–510; E. GΓΆtschi, C. Jenny, P. Reindl, F. Ricklin, Helv. Chim. Acta 1996, 79, 2219–2234 (R1═H; R7═OH); N. A. Sasald, R. Pauli, C. Fontaine, A. Chiaroni, C. Riche, P. Potier, Tetrahedron Lett. 1994, 35, 241–244 (R1═H; R7═COOH); R. Cotton, A. N. C. Johnstone, M. North, Tetrahedron 1995, 51, 8525–8544 (R1═H; R7═COOMe); J. S. Sabol, G. A. Flynn, D. Friedrich, E. W. Huber, Tetrahedron Lett. 1997, 38, 3687–3690 (R1═H; R7═CONH2); P. P. Waid, G. A. Flynn, E. W. Huber, J. S. Sabol, Tetrahedron Lett. 1996, 37, 4091–4094 (R1═H; R1=(4-BnO)C6H4); N. A. Sasaki, R. Pauli, P. Potier, Tetrahedron Lett. 1994, 35, 237–240 (R1═H; R7═SO2Ph); R. J. Heffner, J. Jiang, M. JouilliΓ©, J. Am. Chem. Soc. 1992, 114, 10181–10189; U. Schmidt, H. Griesser, A. Lieberknecht, J. HΓ€usler, Angew. Chem. 1981, 93, 272–273 (R1═H; R7═OAryl); H. Mosberg, A. L. Lomize, C. Wang, H. Kroona, D. L. Heyl, J. Med. Chem. 1994, 37, 4371–4383 (R1═H; R7=4-OHC6H4); S. A. Kolodziej, G. V. Nikiforovich, R. Sceean, M.-F. Lignon, J. Martinez, G. R. Marshall, J. Med. Chem. 1995, 38, 137–149 (R1═H; R7═SCH2(4-Me)C6H4).

A11: See Kuhn, Osswald, Chem. Ber. 1956, 89, 1423–1434; Patchett, Witkop, J. Am. Chem. Soc. 1957, 79, 185–189; Benz, Helv. Chim. Acta 1974, 57, 2459–2475; P. Wessig, Synlett, 1999, 9, 1465–1467; E. M. Smit, G. F. Swiss, B. R. Neustadt, E. H. Gold, J. A. Sommer, J. Med. Chem. 1988, 31, 875–885; J. Krapcho, C. Turk, D. W. Cushman, J. R. Powell, J. M. DeForrest, J. Med. Chem. 1988, 31, 1148 (R1═H; R6═H); D. BenIshai, S. Hirsh, Tetrahedron 1988, 44, 5441–5450 (R1═H; R6═CH3); M. W. Holladay, C. W. Lin, C. S. Garvey, D. G. Witte, J. Med. Chem. 1991, 34, 455–457 (R1═H; R6=alkyl); P. Barralough, P. Hudhomme, C. A. Spray, D. W. Young, Tetrahedron 1995, 51, 4195–4212 (R1═H; R6=Et); J. E. Baldwin, M. Rudolf, Tetrahedron Lett. 1994, 35, 6163–6166; J. E. Baldwin, S. J. Bamford, A. M. Fryer, M. Rudolf, M. E. Wood, Tetrahedron 1997, 53, 5233–5254 (R1═H; R6═CH2COOtBu); P. Gill, W. D. Lubell, J. Org. Chem. 1995, 60, 2658–2659 (R1═H; R6═CH3; Bn; alkyl; CH2COOMe); M. J. Blanco, F. J. Sardina, J. Org. Chem. 1998, 63, 3411–3466 (R1═H; R6═OCH2OMe).

A12: See Ahmed, Cheeseman, Tetrahedron 1977, 33, 2255–2257; J. S. New, J. P. Yevich, J. Heterocycl. Chem. 1984, 21, 1355–1360; R. Kikumoto, Y. Tamao, K. Ohkubo, T. Tezuka, S. Tonomura, J. Med. Chem. 1980, 23, 1293–1299; C. J. Blankley, J. S. Kaltenbronn, D. E. DeJohn, A. Werner, L. R. Bennett, J. Med. Chem. 1987, 30, 992–998; S. Klutcho, C. J. Blankley, R. W. Fleming, J. M. Hinkley, R. E. Werner, J. Med. Chem. 1986, 29, 1953–1961 (R1═H; R8═H); L. J. Beeley, C. J. M. Rockwell, Tetrahedron Lett. 1990, 31, 417–420 (R1═COOEt; R8═H).

A13: See G. Flouret, W. Brieher, T. Majewski, K. Mahan, J. Med. Chem. 1991, 43, 2089–2094; G. Galiendo, P. Grieco, E. Perissuti, V. Santagada, Farmaco, 1996, 51, 197–202; D. F. McComsey, M. J. Hawkins, P. Andrade-Gordon, M. F. Addo, B. E. Maryanoff, Bioorg. Med. Chem. Lett. 1999, 9, 1423–1428; G. B. Jones, S. B. Heaton, B. J. Chapman, M. Guzel, Tetrahedron: Asymmetry 1997, 8, 3625–3636; M. Asami, H. Watanabe, K. Honda, S. Inoue, Tetrahedron: Asymmetry 1998, 9, 4165–4174; K. Gross, Y. M. Yun, P. Beak, J. Org. Chem. 1997, 62, 7679–7689 (R1═H; R6═H; R8═H); K. Gross, Y. M. Yun, P. Beak, J. Org. Chem. 1997, 62, 7679–7689 (R1═H; R6═H; R8=6-Cl); Ch. Noe, M. Knollmueller, C. Schoedl, M. L. Berger, Sci. Pharm. 1996, 64, 577–590; E. Reiman, W. Erdle, H. Unger, Pharmazie, 1994, 54, 418–421 (R1═H; R6═CH2COOH; R8═H); V. Collot, M. Scbmitt, A. K. Marwah, B. Norerg, J.-J. Bourgignon, Tetrahedron Lett. 1997, 38, 8033–8036 (R1═H; R6=Ph; R8═H); L. V. Dunkerton, H. Chen, B. P. McKillican, Tetrahedron Lett. 1988, 29, 2539–2542 (R1═C(CH3)2CH═CH2; R6═H; R8═H); E. J. Corey, J. Am. Chem. Soc. 1970, 92, 2476–2488; Neunhoeffer, Lehmann, Chem. Ber. 1961, 94, 2960–2963 (R1═CH3; R6═H; R8═H).

A14: Amino acids of type A14 can be made according to Scheme 1.

A15: See D. S. Perlow, J. M. Erb, N. P. Gould, R. D. Tung, R. M. Freidinger, J. Org. Chem. 1992, 57, 4394–4400; D. Y. Jackson, C. Quan, D. R. Artis, T. Rawson, B. Blackburn, J. Med. Chem. 1997, 40, 3359–3368 (R1═H; R2═H); H. H. Wasserman, K. Rodrigues, K. Kucharozyl, Tetrahedron Lett. 1989, 30, 6077–6080 (R1═H; R2═COOH).

A16: See Beyerman, Boekee, Recl. Trav. Chim. Pays-Bas, 1959, 78, 648–653; M. E. Freed, A. R. Day, J. Org. Chem. 1960, 25, 2105–2107; D. R. Adams, P. D. Bailey, I. D. Collier, J. D. Heferman, S. Slokes, J. Chem. Soc. Chem. Commun. 1996, 349–350; J. E. Baldwin, R. M. Adlington, C. R. A. Godfrey, D. W. Collins, J. D. Vaughan, J. Chem. Soc. Chem. Commun. 1993, 1434–1435; Y. Matsuanura, Y. Takeshima, H. Ohita, Bull. Chem. Soc. Jpn. 1994, 67, 304–306 (R1═H; R6═H); C. Herdeis, W. Engel, Arch. Pharm. 1991, 324, 670 (R1═COOMe; R6═CH3).

A17, A18: See C. R. Davies, J. S. Davies, J. Chem. Soc. Perkin Trans 1, 1976, 2390–2394; K. Bevan, J. Chem. Soc. C, 1971, 514–522; K. Umezawa, K. Nakazawa, Y. Ikeda, H. Naganawa, S. Kondo, J. Org. Chem. 1999, 64, 3034–3038 (R1═R3═H); P. D. Williams, M. G. Bock, R. D. Tung, V. M. Garsky, D. S. Parlow, J. Med. Chem, 1992, 35, 3905–3918; K. Tamaki, K. Tanzawa, S. Kurihara, T. Oikawa, S. Monma, Chem. Pharm. Bull. 1995, 43, 1883–1893 (R1═R5═H; R3═COOBn); K. J. Hale, J. Cai V. Delisser, S. Manaviazar, S. A. Peak Tetrahedron 1996, 52, 1047–1068; M. H. Chen, O. P. Goel, J.-W. Hyun, J. Magano, J. R. Rubin, Bioorg. Med. Chem. Lett. 1999, 9, 1587–1592 (R1═R5═H; R3═COOtBu); R. Baenteli, I. Brun, P. Hall, R. Metternich, Tetrahedron Lett. 1999, 40, 2109–2112 (R1═R5═H; R3═COR); K. J. Hale, N. Jogiya, S. Manaviazar, Tetrahedron 1998, 39, 7163–7166 (R1═H; R3═COOBn; R5═OBn); T. Kamenecka, S. J. Danishewsky, Angew. Chem. Int. Ed. Engl. 1998, 37, 2995–2998(R1═H; R3═COO(CH2)2SiMe3; R5═OSiMe2tBu.

A19: See Beilstein, Registry Number 648833 (R1═R4═R8═H). Compounds of this type can be prepared according to Scheme 2.

A20: See D. Hagiwara, H. Miyake, N. Igari, M. Karino, Y. Maeda, J. Med. Chem. 1994, 37, 2090–2099 (R1═H; R9═OH); Y. Arakawa, M. Yasuda, M. Ohnishi, S. Yoshifuji, Chem. Pharm. Bull. 1997, 45, 255–259 (R1═H; R9═COOH); P. J. Murray, I. D. Starkey, Tetrahedron Lett. 1996, 37, 1875–1878 (R1═H; R9═(CH2)2NHCOCH2Ph); K. Clinch, A. Vasella, R. Schauer, Tetrahedron Lett. 1987, 28, 6425–6428 (R1═H; R9═NHAc).

A21: See A. Golubev, N. Sewald, K. Burger, Tetrahedron Lett. 1995, 36, 2037–2040; F. Machetti, F. M. Cordero, F. DeSario, A. Guarna, A. Brandi, Tetrahedron Lett. 1996, 37, 4205–4208; P. L. Ornstein, D. D. Schoepp, M. B. Arnold, J. D. Leander, D. Lodge, J. Med. Chem. 1991, 34, 90–97; R1═R6═H); P. D. Leeson, B. J. Williams, R. Baker, T. Ludduwahetty, K. W. Moore, M. Rowley, J. Chem. Soc. Chem. Commun. 1990, 1578–1580; D. I. C. Scopes, N. F. Hayes, D. E. Bays, D. Belton, J. Brain, J. Med. Chem. 1992, 35, 490–501; H. Kessler, M. Kuehn, T. LΓΆschner, Liebigs Ann. Chem. 1986, 1–20 (R1═R6═H); C. Herdeis, W. Engel, Arch. Pharm. 1992, 7, 419–424 (R1═R6=Bn); C. Herdeis, W. Engel, Arch. Pharm. 1992, 411–418 (R1═COOMe; R6═H); C. Herdeis, W. Engel, Arch. Pharm. 1992, 419–424 (R1═COOMe; R6=Bn).

A22: See P. D. Leeson, B. J. Williams, R. Baker, T. Ladduwahetty, K. W. Moore, M. Rowley, J. Chem. Soc. Chem. Comm. 1990, 1578–1580 (R1═H; R10═NHOBn).

A23: See Beyerman, Boekee, Recl. Tray. Chim. Pays-Bas 1959, 78, 648–653; D. R. Adams, P. D. Bailey, I. D. Collier, J. D. Heffernan, S. Stokes J. Chem. Soc. Chem. Commun. 1996, 349–350; J. E. Baldwin, R. M. Adlington, C. Godfrey, D. W. Collins, J. G. Vaughan, J. Chem. Soc. Chem. Comm. 1993, 1434–1435 (R1═R6═H); C. Herdeis, W. Engel, Arch. Pharm. 1993, 297–302 (R1═COOMe; R6═H).

A24: See Plieninger, LeonhΓ€user, Chem. Ber. 1959, 92, 1579–1584; D. W. Knight, N. Lewis, A. C. Share, D. Haigh, J. Chem. Soc. Perkin Trans. 1 1998, 22, 3673–3684; J. Drummond, G. Johnson, D. G. Nickell, D. F. Ortwine, R. F. Bruns, B. Welbaum, J. Med. Chem. 1989, 32, 2116–2128; M. P. Moyer, P. L. Feldman, H. Rapoport, J. Org. Chem. 1985, 50, 5223–5230 (R1═R6═H); McElvain, Laughton, J. Am. Chem. Soc. 1951, 73, 448–451 (R1═H; R6β€”Ph); McElvain, Laughton, J. Am. Chem. Soc. 1951, 73, 448–451 (R1=Ph; R6═H);

A25: See L.-Y. Hu, T. R. Ryder, S. S. Nikam, E. Millerman, B. G. Szoke, M. F. Rafferty, Bioorg. Med. Chem. Lett. 1999, 9, 1121–1126; W. C. Lumma, R. D. Hartman, W. S. Saari, E. L. Engelhardt, V. J. Lotti, C. A. Stone, J. Med. Chem. 1981, 24, 93–101; N. Hosten, M. J. O. Antenuis, Bull. Soc. Chim. Belg. 1988, 97, 48–50; C. F. Bigge, S. J. Hays, P. M. Novak, J. T. Drummond, G. Johnson, T. P. Bobovski, Tetrahedron Lett. 1989, 30, 5193–5191; B. Aebischer, P. Frey, H.-P. Haerter, P. L. Herrling, W. MΓΌller, Helv. Chim. Acta 1989, 72, 1043–1051; W. J. Hoeckstra, B. E. Maryanoff, B. P. Damiano, P. Andrade-Gordon, J. H. Cohen, M. J. Constanzo, B. J. Haertlein, L. R. Hecker, B. L. Hulshizer, J. A. Kaufnan, P. Keane, J. Med. Chem. 1999, 42, 5254–5265 (R1═H; R11═H); B. D. Dorsey, R. B. Levin, S. L. McDaniel, J. P. Vacca, J. P. Guare, J. Med. Chem. 1994, 37, 3443–3451; M. Cheng, B. De, S. Pikul, N. G. Almstaed, M. G. Natchus, M. V. Anastasio, S. J. McPhail, C. J. Snider, Y. O. Taiwo, L. Chen, C. M. Dunaway, J. Med. Chem. 2000, 43, 369–380; R. Kuwano, Y. Ito, J. Org. Chem. 1999, 64, 1232–1237 (R1═H; R11═COOtBu); J. Kitchin, R. C. Bethell, N. Cammack, S. Dolan, D. N. Evans, J. Med. Chem. 1994, 37, 3707–3716 (R1═H; R11═COOPh); C. F. Bigge, S. J. Hays, P. M. Novak, J. T. Drummond, G. Johnson, T. P. Bobovski, J. Med. Chem. 1990, 33, 2916–2924 (R1═H; R11═COOtBu; (CH2)3COOEt; (CH2)3PO(Me)OH; (CH2PO(OH)2; (CH2)2PO(OEt)2; (CH2)2PO(OH)2).

Compounds of type A25 can also be prepared according to Scheme 3:

A26: See Koegel, J. Biol. Chem. 1953, 201, 547 (R1═R12═H).

A27: See G. Makara, G. R. Marshall, Tetrahedron Lett. 1997, 38, 5069–5072; R. N. Patel, A. Banedee, R. L. Hanson, D. B. Brzozowski, L. W. Parker, L. J. Szarka, Tetrahedron: Asymmetry 1999, 10, 31–36 (R1═H; R13═OH, OtBu); J. E. Johanson, B. D. Christie, H. Rapoport, J. Org. Chem. 1981, 46, 4914–4920; N. Moss, J.-S. Duceppe, J.-M- Ferland, J. Gauthier, J. Med. Chem. 1996, 39, 2178–2187 (R1═H; R13═CONHMe); G. M. Makara, G. R. Marshall, Tetrahedron Lett. 1997, 38, 5069–5072 (R1═H; R13═SCH2(4-MeO)C6H4).

A28: See A. Golubev, N. Sewald, K. Burger, Tetrahedron Lett. 1995, 36, 2037–2040; P. L. Ornstein, D. D. Schoepp, M. B. Amold, 3. D. Leander, D. Lodge, J. Med. Chem. 1991, 34, 90–97 (R1═R6═H); P. D. Leeson, B. J. Williams, R. Baker, T. Ladduwahetty, K. W. Moore, M. Rowley, J. Chem. Soc. Chem. Commun. 1990, 22, 1578–1580; C. Herdeis, W. Engel, Arch. Pharm. 1991, 324, 670 (R1═H; R6=Me); C. Herdeis, W. Engel, Arch. Pharm. 1991, 324, 670 (R1═COOMe; R6═H, Me).

A29: See Kawase, Masami, Chem. Pharm. Bull. 1997, 45, 1248–1253; I. G. C. Coutts, J. A. Hadfield, P. R. Huddleston, J. Chem. Res. Miniprint, 1987, 9, 2472–2500; I. G. C. Coutts, J. A. Hadfield, P. R. Huddleston, J. Chem. Res. Miniprint, 1987, 9, 2472–2500; V. J. Hrubi, W. L. Cody, A. M. Castrucci M. E. Hadley, Collect. Czech. Chem. Commun. 1988, 53, 2549–2573; R. T. Shuman, R. B. Rothenberger, C. S. Campbell, G. F. Smith, D. S. Gifford-Moore, P. D. Gesellchen, J. Med. Chem. 1993, 36, 314–319; M. Kawase, Y. Okada, H. Miyamae, Heterocycles, 1998, 48, 285–294 (R1═R8═H); Kawase, Masami, Chem. Pharm. Bull. 1997, 45, 1248–1253 (R1═H; R8=6,7-(MeO2); D. F. Ortwine, T. C. Malone, C. F. Bigge, J. T. Drummond, C. Humblet, J. Med. Chem. 1992, 35, 1345–1370 (R1═H; R8=7-H2PO(OEt)2); E. J. Corey, D. Y. Gin, Tetrahedron Lett. 1996, 37, 7163–7166 (R1═CH2SCOOtBu); P. Dostert, M. Varasi, A. DellaTorre, C. Monti, V. Rizzo, Eur. J. Med. Chim. Ther. 1992, 27, 57–59 (R1=Me; R8=6,7-(OH)2); Z. Czarnocki, D. Suh, D. B. McLean, P. G. Hultin, W. A. Szarek, Can. J. Chem. 1992, 70, 1555–1561; B. SchΓΆnenberger, A. Brossi, Helv. Chim. Acta 1986, 69, 1486–1497 (R1=Me; R8=6-OH; 7-MeO); Hahn, Stiel, Chem. Ber. 1936, 69, 2627; M. Chrzanowska, B. SchΓΆnenberger, A. Brossi, J. L. Flippen-Anderson, Helv. Chim. Acta 1987, 70, 1721–1731; T. Hudlicky, J. Org. Chem. 1981, 46, 1738–1741 (R1=Bn; R8=6,7-(OH)2); A. I. Meyers, M. A. Gonzalez, V. Struzka, A. Akahane, J. Guiles, J. S. Warmus, Tetrahedron Lett. 1991, 32, 5501–5504 (R1═CH2(3,4-methylenedioxy)C6H3; R8=6,7-(OMe)2).

A30 and A31 can be prepared according to Schemes 4 and 5.

A32 can be prepared according to P. W. Schiller, G. Weltrowska, T. M.-D. Nguyen, C. Lemieux, N. Nga, J. Med. Chem. 1991, 34, 3125–3132; V. S. Goodfellow, M. V. Marathe, K. G. Kuhlman, T. D. Fitzpatrick, D. Cuadrato, J. Med. Chem. 1996, 39, 1472–1484; G. Caliendo, F. Fiorino, P. Grieco, E. Perissutti, S. DeLuca, A. Guiliano, G. Santelli, D. Califano, B. Severino, V. Santagada, Farmacao, 1999, 54, 785–790; V. S. Goodfellow, M. V. Marathe, K. G. Kuhlman, T. D. Fitzpatrick, D. Cuadro, J. Med. Chem. 1996, 39, 1472–1484 (R1═R8═H); D. Tourwe, E. Mannekens, N. T. Trang, P. Verheyden, H. Jaspers, J. Med. Chem. 1998, 41, 5167–5176; A.-K. Szardenings, M. Gordeev, D. V. Patel, Tetrahedron Lett. 1996, 37, 3635–3638; W. Wiczk, K. Stachowiak, P. Skurski, L. Lankiewicz, A. Michniewicz, A. Roy, J. Am. Chem. Soc. 1996, 118, 8300–8307; K. Verschuren, G. Toth, D. Tourwe, M. Lebl., G. van Binst, V. Hrubi, Synthesis 1992, 458–460 (R1═H; R8=6-OH); P. L. Ornstein, M. B. Arnold, N. K. Augenstein, J. W. Paschal, J. Org. Chem. 1991, 56, 4388–4392 (R1═H; R8=6-MeO); D. Ma, Z. Ma, A. P. Kozikowski, S. Pshenichlin, J. T. Wroblenski, Bioorg. Med. Lett. 1998, 8, 2447–2450 (R1═H; R8=6-COOH); U. SchΓΆllkopf, R. Hinrichs, R. Lonsky, Angew. Chem. 1987, 99, 137–138 (R1=Me; R8═H); B. O. Kammermeier, U. Lerch, C. Sommer, Synthesis 1992, 1157–1160 (R1═COOMe; R8═H); T. Gees, W. B. Schweizer, D. Seebach, Helv. Chim. Acta 1993, 76, 2640–2653 (R1=Me; R8=6,7-(MeO2).

A33: See Hinton, Mann, J. Chem. Soc. 1959, 599–608.

A34: See G. P. Zecchini, M. P. Paradisi, J. Heterocycl. Chem. 1979, 16, 1589–1597; S. Cerrini, J. Chem. Soc. Perkin Trans. 1, 1979, 1013–1019; P. L. Ornstein, J. W. Paschal, P. D. Gesellchen, J. Org. Chem. 1990, 55, 738–741; G. M. Ksander, A. M. Yan, C. G. Diefenbacher, J. L. Stanton, J. Med. Chem. 1985, 28, 1606–1611; J. A. Robl, D. S. Karanewsky, M. M. Asaad, Tetrahedron Lett. 1995, 36, 1593–1596; S. Katayama, N. Ae, R. Nagata, Tetrahedron: Asymmetry 1998, 9, 4295–4300 (R1═R8═H); K. Hino, Y. Nagai, H. Uno, Chem. Pharm. Bull. 1988, 36, 2386–2400 (R1=Me; R8═H).

A35: See Beilstein Registry Numbers: 530775, 883013 (R1═R8═H).

A36: See R. W. Carling, P. D. Leeson, A. M. Moseley, R. Baker, A. C. Foster, J. Med. Chem. 1992, 35, 1942–1953; S. Kano, T. Ebata, S. Shibuya, J. Chem. Soc. Perkin Trans. 1, 1980, 2105–2111 (R1═R8═H); R. W. Carling, P. D. Leeson, A. M. Moseley, R. Baker, A. C. Foster, J. Med. Chem. 1992, 35, 1942–1953 (R1═H; R8=5-Cl; 7-Cl).

A37: See Nagarajan, Indian J. Chem. 1973, 11, 112 (R1═CH2COOMe; R8═H).

A38: See R. Pauly, N. A. Sasaki, P. Potire, Tetrahedron Lett. 1994, 35, 237–240; J. Podlech, D. Seebach, Liebigs Ann. Org. Bioorg. Chem. 1995, 7, 1217–1228; K. C. Nicolaou, G.-Q. Shi, K. Namoto, F. Bernal, J. Chem. Soc. Chem. Commun. 1998, 1757–1758 (R1═H; R2═H).

A39: See Beilstein, Registry Number 782885.

A40; See F. P. J. C. Rutjes, N. M. Terhuis, H. Hiemstra, N. W. Speckamp, Tetrahedron 1993, 49, 8605–8628 (R1═H; R3=Bn); compounds of this type can be prepared according to Scheme 6.

A41: Compounds of this type can be prepared according to Scheme 7.

A42 to A46: Compounds of this type can be prepared according to Scheme, 8 to 12. Key intermediate 34 and Ξ±-amino acid synthesis involving this building block include: R. M. Williams, M.-N. Im, Tetrahedron Lett. 1988, 29, 6079–6082; R. M. Williams, M.-N. Im, J. Am. Chem. Soc. 1991, 113, 9276–9286; J. F. Dellaria, B. D. Santarsiero, Tetrahedron Lett. 1988, 29, 6079–6082; J. F. Dellaria, B. D. Santarsiero, J. Org. Chem. 1989, 54, 3916–3926; J. E. Baldwin, V. Lee, C. J. Schofield, Synlett 1992, 249–251; J. E. Baldwin, V. Lee, C. J. Schofield, Heterocycles 1992, 34, 903–906.

A47: See P. Barraclough, R. D. Farrant, D. Kettle, S. Smith, J. Chem. Res. Miniprint 1991, 11, 2876–2884 (R1═R11═H, Bn, β€”(CH2)2PO(OEt)2).

A48: See A. Nouvet, M. Binard, F. Lamaty, J. Martinez, R. Lazaro, Tetrahedron 1999, 55, 4685–4698 (R1═R12═H).

A49: See M. Y. Kolleganov, I. G. Kolleganova, M. D. Mitrofanova, L. I. Martynenko, P. P. Nazarov, V. I. Spitsyn, Bull. Acad. Sci. USSR Div. Chem. Sci (Engl. Trans.) 1983, 32, 1293–1299; Izv. Akad. Nauk SSSR Ser. Khim. 1983, 6, 1293–1299; V. P. Vasilev, T. D. Orlova, S. F. Ledenkov, J. Gen. Chem. USSR (Engl. Trans. 1989, 59, 1629–1634; Zh. Obshchi. Khim. 1989, 59, 1828–1833 (R1═H; R12═CH(COOH)CH2COOH). Compounds of type A49 can also be prepared according to Scheme 13.

A50 and A51: Compounds of these types can be prepared according to Schemes 14 and 15.

A53: See P. Barraclough, R. D. Fatrant, D. Kettle, S. Smith, J. Chem. Res. Miniprint 1991, 11, 2876–2884(R1═R11═H; R1═H; R11=Bn, (CH2)3PO(OH)2); β€”(CH2)3PO(Et)2); J. I. Levin, J. F. DiJoseph, L. M. Killar, A. Sung, T. Walter, Bioorg. Med. Chem. Lett. 1998, 8, 2657–2662 (R1═H; R11=4CF3OC6H4CO).

A 52 and A54: Compounds of this type can be prepared according to Schemes 16 and 17.

A55 and A56: Compounds of this type can be prepared according to Schemes 18 and 19.

A57: Compounds of this type can be prepared according to Scheme 20.

A58: See C.-H. Lee, H. Kohn, J. Org. Chem. 1990, 55, 6098–6104 (R1═R8═H).

A59: can be prepared according to Scheme 21.

A60: Compounds of this type can be prepared according to Scheme 22.

A61: See D. R. Armour, K. M. Morriss, M. S. Congreve, A. B. Hawcock, Bioorg. Med. Chem. Lett. 1997, 7, 2037–2042 (R1═R12═H).

A62: Compounds of this type can be prepared according to Scheme 23.

A63: See S. E. Gibson, N. Guillo, R. J. Middleton, A. Thuiliez, M. J. Tozer, J. Chem. Soc. Perkin Trans. 1, 1997, 4, 447–456; S. E. Gibson, N. Guillo, S. B. Kalindjan, M. J. Tozer, Bioorg. Med. Chem. Lett,. 1997, 7, 1289–1292 (R1═H; R8═H); Beilstein Registry Number: 459155 (R1═H; R8=4,5-MeO2).

A64: Compounds of this type can be prepared according to Scheme 24.

A65 and A 67: Compounds of these types can be prepared according to Schemes 25 and 26.

A66: See G. L. Grunewald, L. H. Dahanukar, J. Heterocycl. Chem. 1994, 31, 1609–1618 (R1═H; R8═H, 8-NO2; C(1)=O).

A68: See Griesbeck, H. Mauder, I. MΓΌller, Chem. Ber. 1992, 11, 2467–2476; (R1═R8═H; C(1)═O).

A69: R. Kreher, W. Gerhardt, Liebigs Ann. Chem. 1981, 240–247 (R1═R8═H).

As explained above, building blocks A70 belong to the class of open-chain Ξ±-substituted Ξ±-amino acids, A71 and A72 to the class of the the corresponding Ξ²-amino acid analogues and A73–A104 to the class of the cyclic analogues of A70.

Building blocks of types A70 and A73–A104 have been synthesized by several different general methods: by [2+2] cycloaddition of ketenes with imines (I. Ojima, H. J. C. Chen, X. Quin, Tetrahedron Lett. 1988, 44, 5307–5318); by asymmetric aldol reaction (Y. Ito, M. Sawamura, E. Shirakawa, K. Hayashikazi, T. Hayashi, Tetrahedron Lett. 1988, 29, 235–238; by the oxazolidinone method (J. S. Amato, L. M. Weinstock, S. Karady, U.S. Pat. No. 4,508,921 A; M. Gander-Coquoz, D. Seebach, Helv. Chem. Acta 1988, 71, 224–236; A. K. Beck, D. Seebach, Chimia 1988, 42, 142–144; D. Seebach, J. D. Aebi, M. Gander-Coquoz, R. Naef, Helv. Chim. Acta 1987, 70, 1194–1216; D. Seebach, A. Fadel, Helv. Chim. Acta 1995, 68, 1243–1250; J. D. Aebi, D. Seebach, Helv. Chim. Acta 1985, 68, 1507–1518; A. Fadel, J. Salaun, Tetrahedron Lett. 1987, 28, 2243–2246); by Schmidt- rearrangement of Ξ±,Ξ±-disubstituted Ξ±-ketoesters (G. I. Georg, X. Guan, J. Kant, Tetrahedron Lett. 1988, 29, 403–406); asymmetric synthesis via chiral Ni(II)-derived Schiff-bases (Y. N. Belokon, V. I. Baktmutov, N. I. Chemoglazova, K. A. Kochetov, S. V. Vitt, N. S. Garbalinskaya, V. M. Belikov, J. Chem. Soc. Perkin Trans. 1, 1988, 305–312; M. Kolb, J. Barth, Liebigs Ann. Chem. 1983, 1668–1688); by the bis-lactim ether synthesis (U. SchΓΆllkopf, R. Hinrichs, R. Lonsky, Angew. Chem. 1987, 99, 137–138); by microbial resolution (K. Sakashita, I. Watanabe, JP 62/253397 A2) and by the hydantoin method combined with resolution of the racemic amino acids with chiral auxilliaries derived from L-phenylalanine amides (D. Obrecht, C. Spiegler, P. SchΓΆnholzer, K. MΓΌller, H. Heimgartner, F. Stierli, Helv. Chim. Acta 1992, 75, 1666–1696; D. Obrecht, U. Bohdal, J. Daly, C. Lehmann, P. SchΓΆnholzer, K. MΓΌller, Tetrahedron 1995, 51, 10883–10900; D. Obrecht, C. Lehmann, C. Ruffieux, P. SchΓΆnholzer, K. MΓΌller, Helv. Chim. Acta 1995, 78, 1567–1587; D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580; D. Obrecht, H. Karajiannis, C. Lehmann, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 703–714; D. Obrecht, M. Altorfer, C. Lehmann, P. SchΓΆnholzer, K. MΓΌller, J. Org. Chem. 1996, 61, 4080–4086; D. Obrecht, C. Abrecht, M. Altorfer, U. Bohdal, A. Grieder, P. Pfyffer, K. MΓΌller, Helv. Chim. Acta 1996, 79, 1315–1337). The latter method has been especially useful in preparing both enantiomers of building blocks of type A70 (see Scheme 27) and A73–A104 (see Scheme 28) in pure form.

The method depicted in Scheme 27 consists in treatment of the appropriate ketones 126 with KCN, (NH4)2CO3 in a mixture of ethanol/water (E. Ware, J. Chem. Res. 1950, 46, 403; L. H. Goodson, I. L. Honigberg, J. J. Lehmann, W. H. Burton, J. Org. Chem. 1960, 25, 1920; S. N. Rastogi, J. S. Bindra, N. Anand, Ind. J. Chem. 1971, 1175) to yield the corresponding hydantoins 127, which were hydrolyzed with Ba(OH) in water at 120–140Β° (R. Sarges, R. C. Schur, J. L. Belletire, M. J. Paterson, J. Med. Chem. 1988, 31, 230) to give 128 in high yields. Schotten-Baumann acylation (Houben-Weyl, β€˜Methoden der Organischen Chemie’, Volume XI/2, Stickstoff-Verbindungen II und IIIβ€², Georg Tieme Verlag, Stuttgart, pp 339) followed by cyclization with N,Nβ€²-dicyclohexyl carbodiimide gave azlactones 129 (D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580; D. Obrecht, C. Spiegler, P. SchΓΆnholzer, K. MΓΌller, H. Heimgartner, F. Stierli, Helv. Chim. Acta 1992, 75, 1666–1696). Alternatively, azlactones 129 could also be prepared starting from amino acids 130 and 131, Schotten-Baumann acylation and cyclization with N,Nβ€²-dicyclohexyl carbodimide to azlactones 132 and 133 and alkylation to yield 129 (D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580; D. Obrecht, C. Spiegler, P. SchΓΆnholzer, K. MΓΌller, H. Heimgartner, F. Stierli, Helv. Chim. Acta 1992, 75, 1666–1696)(see Scheme 1). Treatment of 129 with L-phenylalanine cyclohexylamide (D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580) gave diastereomeric peptides 134 and 135, which could be conveniently separated by flash-chromatography or crystallisation. Treatment of 134 and 135 with methanesulphonic acid in methanol at 80Β° gave esters 136a and 136b which were converted into the corresponding Fmoc-protected final building blocks 137a and 137b.

According to the general method described in Scheme 28 (D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580; D. Obrecht, C. Spiegler, P. SchΓΆnholzer, K. MΓΌller, H. Heimgartner, F. Stierli, Helv. Chim. Acta 1992, 75, 1666–1696) A73–A104 can be prepared starting from the corresponding ketones 138, hydantoin formation (139) (E. Ware, J. Chem. Res. 1950, 46, 403; L. H. Goodson, I. L. Honigberg, J. J. Lehmann, W. H. Burton, J. Org. Chem. 1960, 25, 1920; S. N. Rastogi, J. S. Bindra, N. Anand, Ind. J. Chem. 1971, 1175; D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580) and saponification (Ba(OH)2) to yield the racemic amino acids 140, which upon Schotten-Baumann-acylation and cyclization with N,Nβ€²-dicyclohexylcarbodiimide gave azlactones 141. Reaction with L-phenylalanine cyclohexylamide (D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580) gave the diastereomeric peptides 142 and 143, which were separated by flash-chromatography or crystallization. Treatment of 142 and 143 with methanesulphonic acid in methanol at 80Β° gave esters 144a and 144b which were converted into the corresponding suitably protected amino acid precursors 145a and 145b, ready for peptide synthesis.

A71: Amino acid building blocks of this type (see formula 147) can be conveniently prepared from the corresponding disubstituted succinates 146 by Curtius-rearrangement as shown in Scheme 29.

A71: See D. Seebach, S. Abele, T. Sifferlen, M. Haenggi, S. Gruner, P. Seiler, Helv. Chim. Acta 1998, 81, 2218–2243 (R18 and R19 form: β€”(CH2)2β€”; β€”(CH2)3β€”; β€”(CH2)4β€”; β€”(CH2)5β€”; R20═H); L. Ducrie, S. Reinelt, P. Seiler, F. Diederich, D. R. Bolin, R. M. Campbell, G. L. Olson, Helv. Chim. Acta 1999, 82, 2432–2447; C. N. C. Drey, R. J. Ridge, J. Chem. Soc. Perkin Trans. 1, 1981, 2468–2471; U. P. Dhokte, V. V. Khau, D. R. Hutchinson, M. J. Martinelli, Tetrahedron Lett. 1998, 39, 8771–8774 (R18═R19=Me; R20═H); D. L. Varie, D. A. Hay, S. L. Andis, T. H. Corbett, Bioorg. Med. Chem. Lett. 1999, 9, 369–374 (R18═R19=Et); Testa, J. Org. Chem. 1959, 24, 1928–1936 (R18=Et; R19=Ph); M. Haddad, C. Wakselman, J. Fluorine Chem. 1995, 73, 57–60 (R18=Me; R19═CF3; R20═H); T. Shono, K. Tsubata, N. Okinaga, J. Org. Chem. 1984, 49, 1056–1059 (R18═R19═R20=Me); K. Ikeda, Y. Terao, M. Seldya, Chem. Pharm. Bull. 1981, 29, 1747–1749 (R18 and R19 form: β€”(CH2)5β€”; R20=Me).

Amino acid building blocks of type A72 can be conveniently prepared by Arndt-Eistert C1-homologation of compounds of type A70 according to Scheme 30.

A72: See Y. V. Zeifman, J. Gen. Chem. USSR (Engl. Trans.) 1967, 37, 2355–2363 (R18═R19═CF3); W. R. Schoen, J. M. Pisano, K. Pendergast, M. J. Wyvratt, M. H. Fisher, J. Med. Chem. 1994, 37, 897–906; S. Thaisrivongs, D. T. Pals, D. W. DuCharme, S. Turner, G. L. DeGraaf, J. Med. Chem. 1991, 34, 655–642; T. K. Hansen, H. Thoegersen, B. S. Hansen, Bioorg. Med. Chem. Lett. 1997, 7, 2951–2954; R. J. DeVita, R. Bochis, A. J. Frontier, A. Kotliar, M. H. Fisher, J. Med. Chem. 1998, 41, 1716–1728; D. Seebach, P. E. Ciceri, M. Overhand, B. Jaun, D. Rigo, Helv. Chim. Acta 1996, 79, 2043–2066; R. P. Nargund, K. H. Barakat, K. Cheng, W. Chan, B. R. Butler, A. A. Patchett, Bioorg. Med. Chem. Lett. 1996, 6, 1265–1270 (R18═R19=Me); E. Altmann, K. Nebel, M. Mutter, Helv. Chim. Acta 1991, 74, 800–806 (R18=Me; R19═COOMe).

A73: Compounds of this type can be prepared according to C. Mapelli, G. Tarocy, F. Schwitzer, C. H. Stammer, J. Org. Chem. 1989, 54, 145–149 (R21=4-OHC6H4); F. Elrod, E. M. Holt, C. Mapelli, C. H. Stammer, J. Chem. Soc. Chem. Commun. 1988, 252–253 (R21═CH2COOMe); R. E. Mitchell, M. C. Pirrung, G. M. McGeehan, Phytochemistry 1987, 26, 2695 (R21═CH2OH), J. Bland, A. Batolussi, C. H. Stammer, J. Org. Chem. 1988, 53, 992–995 R21═CH2NH2). Additional derivatives of A73 have been described by T. Wakamiya, Y. Oda, H. Fujita, T. Shiba, Tetrahedron Lett. 1986, 27, 2143–2134; U. SchΓΆllkopf, B. Hupfeld, R Gull, Angew. Chem. 1986, 98, 755–756; J. E. Baldwin, R. M. Adlington, B. J. Rawlings, Tetrahedron Lett. 1985, 26, 481–484; D. Kalvin, K. Ramalinggar, R. Woodard, Synth. Comm. 1985, 15, 267–272 and L. M. Izquierdo, I. Arenal, M. Bemabe, E. Alvarez, Tetrahedron Lett. 1985, 41, 215–220.

A74: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding cyclobutanones.

A75 and A76: Compounds of this type can be prepared using the following methods: P. Hughes, J. Clardy, J. Org. Chem. 1988, 53, 4793–4796; E. A. Bell, M. Y. Qureshi, R. J. Pryce, D. H. Janzen, P. Lemke, J. Clardy, J. Am. Chem. Soc. 1980, 102, 1409; Y. Gaoni, Tetrahedron Lett. 1988, 29, 1591–1594; R. D. Allan, J. R. Haurahan, T. W. Hambley, G. A. R. Johnston, K. N. Mewett, A. D. Mitrovic, J. Med. Chem. 1990, 33, 2905–2915 (R23═COOH); G. W. Fleet, J. A. Seijas, M. Vasquez Tato, Tetrahedron 1988, 44, 2077–2080 (R23═CH2OH).

A77: Compounds of this type can be prepared according to J. H. Burcihalter, G. Schmied, J. Pharm. Sci. 1966, 55, 443–445 (R23=aryl).

A78: Compounds of this type can be prepared according to J. C. Watkins, P. Kroosgard-Larsen, T. HonorΓ©, TIPS 1990, 11, 25–33; F. Trigalo, D. Brisson, R. Azerad, Tetrahedron Lett. 1988, 29, 6109 (R24═COOH).

A79: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding pyrrolidine-3-ones.

A80–A82: Compounds of this type can be prepared according to D. M. Walker, E. W. Logusch, Tetrahedron Lett. 1989, 30, 1181–1184; Y. Morimoto, K. Achiwa, Chem. Pharm. Bull. 1989, 35, 3845–3849; J. Yoshimura, S. Kondo, M. Ihara, H. Hashimoto, Carbohydrate Res. 1982, 99, 129–142.

A83: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding pyrazoline-4-ones.

A84: Compounds of this type can be prepared according to R. M. Pinder, B. H. Butcher, D. H. Buxton, D. J. Howells, J. Med. Chem. 1971, 14, 892–893; D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580.

A85: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding indane-1,3-diones.

A86: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding indane-2-ones.

A87: Compounds of this type and analogues thereof can be prepared according to C. Cativiela, M. D. Diaz de Villegas, A. Avenoza, J. M. Peregrina, Tetrahedron 1993, 47, 10987–10996; C. Cativiela, P. Lopez, J. A. Mayoral, Tetrahedron Assymmetry 1990, 1, 379; C. Cativiela, J. A. Mayoral, A. Avenoza, M. Gonzalez, M. A. Rey, Synthesis 1990, 1114.

A87 and A88: Compounds of this type can be prepared according to L. Munday, J. Chem. Soc. 1961, 4372; J. Ansell, D. Morgan, H. C. Price, Tetrahedron Lett. 1978, 47, 4615–4616.

A89: Compounds of this type can be prepared according to general method described in Scheme 28 stating from the corresponding piperidine-3-ones.

A90: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding tetahydrothiapyran-3-ones.

A91: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding tetrahydropyran-3-ones.

A92: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding piperidine-2,5-diones.

A93: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding cyclohexanones.

A94: Compounds of this type can be prepared according to J. Org. Chem. 1990, 55, 4208.

A95: Compounds of this type can be prepared according to N. J. Lewis, R. L. Inloes, J. Hes, R. H. Matthews, G. Milo, J. Med. Chem. 1978, 21, 1070–1073.

A96: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding tetrahydropyran-4-ones.

A97: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding piperidine-2,4-diones.

A98: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding 1-tetralones (D. Obrecht, C. Spiegler, P. SchΓΆnholzer, K. MΓΌller, H. Heimgartner, F. Stierli, Helv. Chim. Acta 1992, 75, 1666–1696).

A99: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding tetraline-1,4-dione mono-diethylacetals.

A100: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding tetrahydroquinolin-4-ones.

A101: Compounds of this type can be prepared according to general method described in Scheme 28 starting from the corresponding tetrahydroquinoline-2,4-diones.

A102: Compounds of this type can be prepared according to K. Ishizumi, N. Ohashi, N. Tanno, J. Org. Chem. 1987, 52, 4477–4485; D. Obrecht, U. Bohdal, C. Broger, D. Bur, C. Lehmann, R. Ruffieux, P. SchΓΆnholzer, C. Spiegler, Helv. Chim. Acta 1995, 78, 563–580; D. Obrecht, C. Spiegler, P. SchΓΆnholzer, K. MΓΌller, H. Heimgartner, F. Stierli, Helv. Chim. Acta 1992, 75, 1666–1696; D. R. Haines, R. W. Fuller, S. Ahmad, D. T. Vistica, V. E. Marquez, J. Med. Chem. 1987, 30, 542–547; T. Decks, P. A. Crooks, R. D. Waigh, J. Pharm. Sci 1984, 73, 457–460; I. A. Blair, L. N. Mander, Austr. J. Chem. 1979, 32, 1055–1065.

Overviews dealing with building blocks of types (b)–(p) are: S. Hanessian, G. McNaughton-Smith, H.-G. Lombart, W. D. Lubell, Tetrahedron 1997, 38, 12789–12854; D. Obrecht, M. Altorfer, J. A. Robinson, β€œNovel Peptide Mimetic Building Blocks and Strategies for Efficient Lead Finding”, Adv. Med. Chem. 1999, Vol. 4, 1–68

Templates of type (b1) can be prepared according to Schemes 31 and 32.

  • i: Treatment of 150 with a dehydrating reagent such as thionylchloride in methanol at an elevated temperature, conveniently at reflux.
  • ii: Introduction of Boc, e.g. using di-tert.butyl dicarbonate and triethylamine in a suitable solvent such as dichloromethane; any other suitable N-protecting group (not shown in Reaction Scheme 31) can be introduced in an analogous manner.
  • iii: Reaction of formed product with phthalimide, diethyl diazodicarboxylate and triphenylphoshine under standard Mitsunobu conditions (Mitsunobu, O.; Wada, M.; Sano, T. J. J. Am. Chem. Soc. 1972, 94, 672) to conveniently yield 151.
  • iv: Treatment of 151 with trifluoracetic acid in dichloromethane.
  • v: 152 is coupled under standard peptide coupling conditions with Cbz-Asp(tBu)OH in DMF with reagents such as HBTU and 1-hydroxybenztriazole (HOBt) with a base such as diisopropylethylamine to yield 153.
  • vi: Removal of the Cbz-group, conveniently by hydrogenation using H2 and a catalyst such as Palladium on charcoal, in solvents such as ethanol, DMF and ethyl acetate.
  • vii: The phthalimide group is cleaved off from the resulting product, conveniently by treatment with hydrazine in a suitable solvent such as ethanol at an elevated temperature, suitably at about 80Β° C. and cleavage of the formed product with trifluoracetic acid in CH2Cl2.
  • viii: The formed amino acid is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succininide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 154 as described by Bisang, C.; Weber, C.; Robinson, J. A. Helv. Chim. Acta 1996, 79, 1825–1842.

  • i: Treatment of 150 with a dehydrating reagent such as thionyl chloride in a suitable solvent such as methanol at an elevated temperature, conveniently at reflux.
  • ii: The resulting amino acid ester is N-protected under standard conditions for introducing the Cbz-group, e.g. using benzyloxycarbonyl chloride and triethylamine in a suitable solvent such as dichloromethane.
  • iii: The Cbz-protected amino acid methyl ester is treated with trimethylsilylchloride and a base such as triethylamine in a solvent such as tetrahydrofuran, cooled, conveniently to about βˆ’78Β° C., followed by reaction with a strong base such as lithium diisopropylamide or lithium hexamethyldisilylazide and tert.-butyl bromoacetate yielding 155 as a mixture of diastereomers as described by Bisang, C.; Jiang, L.; Freund, E.; Emery, F.; Bauch, C.; Matile, H,; Pluschke, G.; Robinson, J. A. J. Am. Chem. Soc. 1998, 120, 7439–7449; Emery, F.; Bisang, C.; Favre, M.; Jiang, L.; Robinson, J. A. J. Chem. Soc. Chem. Commun. 1996, 2155–2156.
  • iv: Reaction of 155 with phthalimide, diethyl diazodicarboxylate and triphenylphosphine under standard Mitsunobu conditions (Mitsunobu, O.; Wada, M.; Sano, T. J. J. Am. Chem. Soc. 1972, 94, 672).
  • v: The resulting product is hydrogenated using H2 and a suitable catalyst such as palladium on charcoal in a solvent such as ethyl acetate, DMF or ethanol; subsequently separation of diastereomers takes place and yields 156.
  • vi: 156 is coupled with Fmoc-Asp(alkyl)OH under standard peptide coupling conditions using reagents such as HATU, HOAt and a base such as diisopropylethylamine in a suitable solvent such as DMF.
  • vii: Cyclization, conveniently with DBU in DMF to yield 157.
  • viii: The phthalimide group is cleaved off from resulting product, conveniently by hydrazinolysis, e.g. treatment with methylhydrazine in a suitable solvent such as DMF.
  • ix: The formed product is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbanyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 158.
  • x: Standard removal of an alkyl ester group using e.g. palladium(0) as catalyst gives 159.

Templates of type (b2) can be prepared according to Scheme 33.

  • i: 160 (obtainable from Vitamin C as described by Hubschwerlen, C. (Synthesis 1986, 962) is treated with phthalimide, diethyl diazodicarboxylate and triphenylphoshine under standard Mitsunobu conditions (Mitsunobu, O.; Wada, M.; Sano, T. J. J. Am. Chem. Soc. 1972, 94, 672).
  • ii: The phthalimide group is cleaved off from the product, conveniently by hydrazinolysis, e.g. by treatment with methylhydrazine in a suitable solvent such as DMF.
  • iii: The amino group is protected by treatment with a benzoylating reagent such as benzoic acid anhydride or benzoylchloride and a base such as triethylamine or 4-dimethylaminopyridine in a suitable solvent such as dichloromethane or DMF.
  • iv: Removal of the 2,4-dimethoxybenzyl group, e.g. with K2S2O8 and Na2HPO4 in aqueous acetonitrile at an elevated temperature, e.g. at about 80Β° C.
  • v: Introduction of a tert.-butoxycarbonyl group using e.g. di-tert.-butyloxycarbonyl dicarbonate, triethylamine and a catalytic amount of 4-dimethylaminopyridine in a suitable solvent such as dichloromethane.
  • vi: Reaction with aqueous sodium carbonate in tetrahydrofuran followed by acidification.
  • vii: Esterification of the carboxylic acid group, conveniently with diazomethane in a suitable solvent such as diethylether yielding 161.
  • viii Removal of the Cbz-group, conveniently by hydrogenation with H2 in the presence of a catalyst such as palladium on charcoal in a solvent such as DMF to yield 161 as described by Pfeifer, M.; Robinson, J. A. J. Chem. Soc. Chem. Commun. 1998, 1977.
  • ix: 161 is coupled under standard peptide coupling conditions with Cbz-Asp(tBu)OH in DMF with reagents such as HBTU and 1-hydroxybenztriazole with a base such as diisopropylethylamine to yield 162 as described by Pfeifer, M.; Robinson, J. A. J. Chem. Soc. Chem. Commun. 1998, 1977.
  • x: Removal of the Cbz-group, e.g. by hydrogenation using H2 and a catalyst such as palladium on charcoal under standard conditions, yields 163 as described by Pfeifer, M.; Robinson, J. A, J. Chem. Soc. Chem. Commun. 1998, 1977.
  • xi: Cleavage of the tert.-butyl ester and tert.-butyloxycarbonyl groups, conveniently using trifluoracetic acid in dichloromethane or 4N hydrochloric acid in dioxane.
  • xii: The intermediate free amino acid formed is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 164 as described by Pfeifer, M.; Robinson, J. A. J. Chem. Soc. Chem. Commun. 1998, 1977.

Templates of type (c1) can be prepared according to Schemes 34 to 37.

  • i: 166 can be synthesized from 165 according to P. Waldmeier, β€œSolid-supported synthesis of highly substituted xanthene-derived templates for the synthesis of Ξ²-turn stabilized cyclic peptide libraries”, PhD-thesis, University of Zurich, 1996. For cleaving the phthalimide group 166 is conveniently submitted to hydrazinolysis, e.g. by treatment with hydrazine hydrate in a suitable solvent such as ethanol at an elevated temperature, e.g. at about 80Β° C.
  • ii: The intermediate aminonitrile is saponified, conveniently under basic conditions, e.g. with aqueous sodium hydroxide in a suitable solvent such as ethanol at an elevated temperature, conveniently under reflux, to yield 167.
  • iii: The intermediate free amino acid formed is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 168 as described by P. Waldmeier, β€œSolid-supported synthesis of highly substituted xanthene-derived templates for the synthesis of Ξ²-turn stabilized cyclic peptide libraries”, PhD-thesis, University of Zurich, 1996.
  • iv: Regioselective bromination of 167 is performed preferably with bromine in acetic acid and dichloromethane. In a similar fashion R37═NO2 can be introduced by treatment with HNO3 in acetic acid and R37═CH2β€”NPht by treatment with hydroxymethyl phthalimide in H2SO4.
  • v: The amino group is conveniently Cbz-protected with reagents such as benzyloxycarbonyl chloride or succinimide in a suitable solvent such as dioxane in presence of a base such as aqueous sodium hydroxide.
  • vi: The carboxylic acid group is esterified, preferably with DBU and methyl iodide in DMF to yield 169.
  • vii: Introduction of lower alkyl, substituted lower alkyl and aryl substituents (R37), conveniently by palladium(0)-catalyzed Stille-(Stille, J. K. Angew. Chem. 1986, 68, 504) and Suzuki-couplings (Oh-e, T.; Mijaura, N.; Suzuki, A. J. Org. Chem. 1993, 58, 2201). Any other functionalization known for aryl bromides can be employed for introduction of substituents R37.
  • viii: Removal of the Cbz-group, e.g. by hydrogenation using H2 and a catalyst such as palladium on charcoal in a suitable solvent such as ethanol, DMF and ethyl acetate.
  • ix: Hydrolysis of the ester group, conveniently under acidic conditions, e.g. with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, preferably at about 100Β° C.
  • x: The intermediate free amino acid formed is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 170.

  • i: Double ortho-bromination of 171 is performed preferably with excess bromine in acetic acid and dichloromethane. In a similar fashion R37═R38═NO2 can be introduced by treatment with HNO3 in acetic acid and R37═R38═CH2β€”NPht by treatment with hydroxymethyl phthalimide in H2SO4.
  • ii: The amino group is protected, conveniently Cbz-protected, with reagents such as benzyloxycarbonyl chloride or succinimide in a suitable solvent such as dioxane in the presence of a base such as aqueous sodium hydroxide.
  • iii: The carboxylic acid group is esterified, preferably with DBU and methyl iodide in DMF to yield 172.
  • iv: Introduction of lower alkyl, substituted lower alkyl and aryl substituents (R37═R38), e.g. by palladium(0)-catalyzed Stille-(Stifle, J. K. Angew. Chem. 1986, 68, 504) and Suzuki-couplings (Oh-e, T.; Mijaura, N.; Suzuki, A. J. Org. Chem. 1993, 58, 2201). Any other functionalization known for aryl brormides can be employed for introduction of substituents R37 and R38.
  • v: Removal of the Cbz-group of 173, e.g. by hydrogenation using H2 and a catalyst such as palladium on charcoal in a suitable solvent such as ethanol, DMF or ethyl acetate.
  • vi: Hydrolysis of the ester group, conveniently under acidic conditions, e.g. with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, conveniently at about 100Β° C.
  • vii: The intermediate free amino acid formed is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 174.

  • i: Cleavage of the methoxy groups of 166, preferably by treatment with an excess of boron tribromide in a suitable solvent such as dichloromethane.
  • ii: Hydrolysis of the cyano group under acidic conditions, preferably with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, conveniently at about 100Β° C.
  • iii: The resulting acid is treated with a dehydrating agent such as thionyl chloride in a suitable solvent such as dioxane to yield 175.
  • iv: Treatment of 175 with an appropriate triflating reagent, preferably trifluoromethanesulfonic acid anhydride in the presence of a base such as 2,6-di-tert.-butyl-pyridine in a suitable solvent such as dichloromethane.
  • v: Heating of the intermediate, conveniently in a suitable solvent such as methanol.
  • vi: Introduction of lower alkyl or aryl-lower alkyl (R35) by alkylation to yield 177. Any other functionalization known for phenol groups can be employed for introduction of substituents R35.
  • vii: Introduction of lower alkyl or aryl (R36), conveniently by palladium(0)-catalyzed Suzuki-coupling (Ohe, T.; Mijaura, N.; Suzuki, A. J. Org. Chem. 1993, 58, 2201) to yield 178. Any other functionalization known for aryl bromides can be employed for introduction of substituents R36.
  • viii: Hydrolysis of the ester group under acidic conditions, conveniently with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, e.g. at about 100Β° C.
  • ix: Cleavage of the phthalimido group, conveniently by hydrazinolysis, e.g. with hydrazine hydrate in a suitable solvent such as ethanol.
  • x: The intermediate free amino acid formed is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 179.

  • i: Bromination of 175 using reagents such as bromine in a mixture of acetic acid and dichloromethane at temperatures ranging from about 0Β° C. to about room temperature.
  • ii: Benzoylation of the hydroxy group using an appropriate acylating agent such as benzoyl chloride or benzoic acid anhydride, a base such as pyridine or triethylamine and a suitable solvent such as dichloromethane to yield 180.
  • iii: 180 is treated with methanol and a catalytic amount of an acidic catalyst such as camphor sulfonic acid under heating.
  • iv: Introduction of lower alkyl or aryl-lower alkyl (R35) by alkylation using a base such as sodium hydride or potassium tert.-butoxide in a solvent such as tetrahydrofuran, dimethoxyethane or DMF gives 181.
  • v: Lower alkyl, substituted lower alkyl and aryl substituents (R38) are introduced, e.g. by palladium(0)-catalyzed Stille-(Stille, J. K. Angew. Chem. 1986, 68, 504) and Suzuki-couplings (Oh-e, T.; Mijaura, N.; Suzuki, A. J. Org. Chem. 1993, 58, 2201). Any other functionalization known for aryl bromides can be employed for introduction of substituents R38.
  • vi: For cleaving the benzyloxy group the intermediate is conveniently heated with sodium cyanide adsorbed on aluminum oxide and methanol.
  • vii: Treatment with an appropriate triflating reagent, preferably trifluoromethanesulfonic acid anhydride, in the presence of a base such as 2,6-di-tert-butyl-pyridine in a suitable solvent such as dichloromethane.
  • viii: Introduction of lower alkyl and aryl substituents (R36), e.g. by palladium(0)-catalyzed Stille-(Stille, J. K. Angew. Chem. 1986, 68, 504) and Suzuki-couplings (Oh-e, T.; Mijaura, N.; Suzuki, A. J. Org. Chem. 1993, 58, 2201) yields 182. Any other functionalization known for aryl bromides can be employed for introduction of substituents R36.
  • ix: Bromination under standard conditions such as using bromine in acetic acid and dichloromethane at temperatures ranging from about 0Β° C. to about room temperature.
  • x: Lower alkyl, substituted lower alkyl and aryl substituents (R37) are introduced, e.g. by palladium(0)-catalyzed Stille-(Stille, J. K. Angew. Chem. 1986, 68, 504) and Suzuki-couplings (Oh-e, T.; Mijaura, N.; Suzuki, A. J. Org. Chem. 1993, 58, 2201) to yield 184. Any other functionalization known for aryl bromides can be employed for introduction of substituents R37.
  • xi: The ester group is hydrolyzed under acidic conditions, conveniently with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, e.g. at about 100Β° C.
  • xii: The phthalimido group is cleaved, e.g. by hydrazinolysis, conveniently with hydrazine hydrate in a suitable solvent such as ethanol.
  • xiii: The intermediate free amino acid formed is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 185.

Templates of type (c2) can be prepared as shown in Schemes 38 and 39.

  • i: 3,7-Dimethoxyphenothiazine 186 is prepared and converted into 187 according to MΓΌller, K.; Obrecht, D.; Knierzinger, A.; Spiegler, C.; Bannwarth, W.; Trzeciak, A.; Englert, G.; Labhardt, A.; SchΓΆnholzer, P. Perspectives in Medicinal Chemistry, Editor Testa, B.; Kyburz, E.; Fubrer, W.; Giger, R., Weinheim, New York, Basel, Cambridge: Verlag Helvetica Chimica Acta, 1993, 513–531; Bannwarth, W.; Gerber, F.; Grieder, A.; Knierzinger, A.; MΓΌller, K.; Obrecht. D.; Trzeciak, A. Can. Pat. Appl. CA2101599(131 pages). The benzyl group is cleaved off from 187 conveniently by hydrogenation, e.g. with H2 and a catalyst such as palladium on charcoal in a suitable solvent such as ethanol, DMF or ethyl acetate.
  • ii: Introduction of lower alkyl (R43) by alkylation using an appropriate alkylating agent (R43β€”Xβ€²; X′═OTf, Br, I) and strong bases such as sodium amide in liquid ammonia or sodium hydride in tetrahydrofuran, dioxan or DMF in the presence of a phase transfer catalyst such as TDA-I. In a similar manner substituted lower alkyl (R43) can be introduced; thus, for example R43═CH2COOR55 and CH2CH2COOR55 can be introduced by treatment with the appropriate 2-halo acetic and, respectively, 3-halo propionic acid derivatives. Any other functionalization known for diarylamines can be employed for introduction of substituents R43.
  • iii: Cleavage of the methoxy groups of 188, conveniently by treatment with an excess of boron tribromide in a suitable solvent such as dichloromethane at temperatures ranging from about βˆ’20Β° C. to about room temperature.
  • iv: For the introduction of lower alkyl, substituted lower alkyl or aryl-lower alkyl substituents (R39 and R40) the intermediate bis-phenol derivative is conveniently reacted with a reagent of the formula R39β€” and R40β€”Xβ€² (X′═OTf, Br, I) in the presence of strong bases such as sodium hydride in tetrahydrofuran, dioxan or DMF in the presence of a phase transfer catalyst such as TDA-I. Any other functionalization known for phenol groups can be employed for introduction of substituents R39 and R40.
  • v: The cyano group of 188 and, respectively, 189 is hydrolyzed, conveniently under acidic conditions, e.g. with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, e.g. at about 100Β° C.
  • vi: The phthalimide group of the intermediate is cleaved, conveniently by hydrazinolysis, e.g. with hydrazine hydrate in a suitable solvent such as ethanol.
  • vii: The free amino group is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 190 and, respectively, 191.

  • i: The cyano group of 188 is hydrolyzed, conveniently under acidic conditions, e.g. with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, e.g. at about 100Β° C.
  • ii: The phthalimide group of the intermediate is cleaved, conveniently by hydrazinolysis, e.g. with hydrazine hydrate in a suitable solvent such as ethanol to yield 192.
  • iii: Double ortho-bromination of 192 is performed preferably with excess bromine in acetic acid and dichloromethane. In a similar fashion R41═R42═NO2 can be introduced by treatment with HNO3 in acetic acid and R41═R42═CH2β€”NPht by treatment with hydroxymethyl phthalimide in H2SO4. Any other functionalization by electrophilic aromatic substitution known can be employed for introduction of substituents R41 and R42.
  • iv: The amino group is protected, conveniently Cbz-protected, with reagents such as benzyloxycarbonyl chloride or succinimide in a suitable solvent such as dioxane in the presence of a base such as aqueous sodium hydroxide.
  • v: The carboxylic acid group is esterified, preferably with DBU and methyl iodide in DMF to yield 193.
  • vi: Regioselective bromination of 192 is performed preferably with bromine in acetic acid and dichloromethane. In a similar fashion R41═NO2 can be introduced by treatment with HNO3 in acetic acid and R41═CH2β€”NPt by treatment with hydroxymethyl phthalimide in H2SO4. Any other functionalization by electrophilic aromatic substitution known can be employed for introduction of substituents R41.
  • vii: The amino group is conveniently Cbz-protected with reagents such as benzyloxycarbonyl chloride or succinimide in a suitable solvent such as dioxane in presence of a base such as aqueous sodium hydroxide.
  • viii: The carboxylic acid group is esterified, preferably with DBU and methyl iodide in DMF to yield 194.
  • ix: Introduction of lower alkyl, substituted lower alkyl and aryl substituents (R41) for 194 and (R41 and R42) for 193, conveniently by palladium(0)-catalyzed Stille-(Stille, J. K. Angew. Chem. 1986, 68, 504) and Suzuki-couplings (Oh-e, T.; Mijaura, N.; Suzuki, A. J. Org. Chem. 1993, 58, 2201). Any other functionalization known for aryl bromides can be employed for introduction of substituents R41 and R42.
  • x: Removal of the Cbz-group, e.g. by hydrogenation using H2 and a catalyst such as palladium on charcoal in a suitable solvent such as ethanol, DMF and ethyl acetate.
  • xi: Hydrolysis of the ester group, conveniently under acidic conditions, e.g. with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, preferably at about 100Β° C.
  • xii: The intermediate free amino acid formed is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 195 and 196.

Templates of type (c3) can be prepared as shown in Schemes 40 and 41.

  • i: 197 can be prepared from commercial resorufin and coverted into 198 according to MΓΌller, K.; Obrecht, D.; Knierzinger, A.; Spiegler, C.; Bannwarth, W.; Trzeciak, A.; Englert, G.; Labhardt, A.; SchΓΆnholzer, P. Perspectives in Medicinal Chemistry, Editor Testa, B.; Kyburz, E.; Fubrer, W.; Giger, R., Weinheim, New York, Basel, Cambridge: Verlag Helvetica Chimica Acta, 1993, 513–531; Bannwarth, W.; Gerber, F.; Grieder, A.; Knierzinger, A.; MΓΌller, K.; Obrecht. D.; Trzeciak, A. Can. Pat. Appl. CA2101599(131 pages). For splitting off the benzyl group 198 is conveniently hydrogenated e.g. with H2 and a catalyst such as palladium on charcoal in a suitable solvent such as ethanol, DMF or ethyl acetate.
  • ii: Introduction of lower alkyl (R43) by alkylation with R43β€”Xβ€² (X′═OTf, Br, I) using strong bases such as sodium amide in liquid ammonia or sodium hydride in tetrahydrofuran, dioxan or DMF in the presence of a phase transfer catalyst such as TDA-I to yield 199. In a similar manner substituted lower alkyl (R43) can be introduced; thus, for example, R43═CH2COOR55 and CH2CH2COOR55 can be introduced by treatment with the appropriate 2-halo acetic and, respectively, 3-halo propionic acid derivatives. Any other functionalization of diarylamino groups known can be employed for introduction of substituents R43.
  • iii: Cleavage of the methoxy groups of 199, conveniently by treatment with excess boron tribromide in dichloromethane at temperatures ranging from about βˆ’20Β° to about room temperature.
  • iv: The intermediate bis-phenol derivative is preferably reacted with R39 and R40β€”Xβ€² (X′═OTf, Br, I) in the presence of strong bases such as sodium hydride in tetrahydrofuran, dioxan or DMF in the presence of a phase transfer catalyst such as TDA-I. Any other functionalization for phenol groups can be employed for introduction of substituents R39 and R40.
  • v: The cyano group of 199 and, respectively, 200 is hydrolyzed under acidic conditions, e.g. with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, conveniently at about 100Β° C.
  • vi: The phthalimide group is cleaved, conveniently by hydrazinolysis, e.g. with hydrazine hydrate in suitable solvent such as ethanol.
  • vii: The free amino group is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 201 and, respectively, 202.

  • i: The cyano group of 199 is hydrolyzed, conveniently under acidic conditions, e.g. with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, e.g. at about 100Β° C.
  • ii: The phthalimide group of the intermediate is cleaved, conveniently by hydrazinolysis, e.g. with hydrazine hydrate in a suitable solvent such as ethanol to yield 203.
  • iii: Double ortho-bromination of 203 is performed preferably with excess bromine in acetic acid and dichloromethane. In a similar fashion R41═R42═NO2 can be introduced by treatment with HNO3 in acetic acid and R41═R42═CH2β€”NPht by treatment with hydroxymethyl phthalimide in H2SO4. Any other functionalization by electrophilic aromatic substitution can be employed for introduction of substituents R41 and R42.
  • iv: The amino group is protected, conveniently Cbz-protected, with reagents such as benzyloxycarbonyl chloride or succinimide in a suitable solvent such as dioxane in the presence of a base such as aqueous sodium hydroxide.
  • v: The carboxylic acid group is esterified, preferably with DBU and methyl iodide in DMF to yield 204.
  • vi: Regioselective bromination of 203 is performed preferably with bromine in acetic acid and dichloromethane. In a similar fashion R41═NO2 can be introduced by treatment with HNO3 in acetic acid and R41═CR2β€”NPht by treatment with hydroxymethyl phthalimide in H2SO4.
  • vii: The amino group is conveniently Cbz-protected with reagents such as benzyloxycarbonyl chloride or succinimide in a suitable solvent such as dioxane in presence of a base such as aqueous sodium hydroxide.
  • viii: The carboxylic acid group is esterified, preferably with DBU and methyl iodide in DMF to yield 205.
  • ix: Introduction of lower alkyl, substituted lower alkyl and aryl substituents (R41) for 205 and (R41 and R42) for 204, conveniently by palladium(0)-catalyzed Stille-(Stille, J. K. Angew. Chem. 1986, 68, 504) and Suzuki-couplings (Oh-e, T.; Mijaura, N.; Suzuki, A. J. Org. Chem. 1993, 58, 2201). Any other functionalization known for aryl bromides can be employed for introduction of substituents R41 and R42.
  • x: Removal of the Cbz-group, e.g. by hydrogenation using H2 and a catalyst such as palladium on charcoal in a suitable solvent such as ethanol, DMF and ethyl acetate.
  • xi: Hydrolysis of the ester group, conveniently under acidic conditions, e.g. with 25% aqueous hydrochloric acid in a suitable solvent such as dioxane at an elevated temperature, preferably at about 100Β° C.
  • xii: The intermediate free amino acid formed is conveniently protected with reagents such as 9-fluorenylmethoxcarbonyl chloride or 9-fluorenylmethoxcarbonyl succinimide using a base such as sodium carbonate or triethylamine in a suitable solvent or mixture of solvents such as dioxane and water, or dichloromethane to yield 206 and 207.

Templates(d) can be prepared according to D. Obrecht, U. Bohdal, C. Lehmann, P. SchΓΆnholzer, K. MΓΌller, Tetrahedron 1995, 51, 10883; D. Obrecht, C. Abrecht, M. Altorfer, U. Bohdal, A. Grieder, M. Kleber, P. Pfyffer, K. MΓΌller, Helv. Chim. Acta 1996, 79, 1315–1337.

Templates (e1) and (e2): See R. Mueller, L. Revesz, Tetrahedron Lett. 1994, 35, 4091; H.-G. Lubell, W. D. Lubell, J. Org. Chem. 1996, 61, 9437; L. Colombo, M. DiGiacomo, G. Papeo, O. Carugo, C. Scolastico, L. Manzoni, Tetrahedron Lett. 1994, 35, 4031.

Templates (e3): See S. Hanessian, B. Ronan, A. Laoui, Bioorg. Med. Chem. Lett. 1994, 4, 1397.

Templates (e4): See S. Hanessian, G. McNaughton-Smith, Bioorg. Med. Chem. Lett. 1996, 6, 1567.

Templates (f): See T. P. Curran, P. M. McEnay, Tetrahedron Lett. 1995, 36, 191–194.

Templates (g): See D. Gramberg, C. Weber, R. Beeli, J. Inglis, C. Bruns, J. A. Robinson, Helv. Chem. Acta 1995, 78, 1588–1606; K. H. Kim, J. P. Dumas, J. P. Germanas, J. Org. Chem. 1996, 61, 3138–3144.

Templates (h): See S. de Lombart, L. Blanchard, L. B. Stamford, D. M. Sperbeck, M. D. Grim, T. M. Jenson, H. R. Rodriguez, Tetrahedron Lett. 1994, 35, 7513–7516.

Templates (i1): See J. A. Robl, D. S. Karanewski, M. M. Asaad, Tetrahedron Lett. 1995, 5, 773–758.

Templates (i2): See T. P. Burkholder, T.-B. Le, E. L. Giroux, G. A. Flynn, Bioorg. Med. Chem. Lett. 1992, 2, 579.

Templates (i3) and (i4): See L. M. Simpkins, J. A. Robl, M. P. Cimarusti, D. E. Ryono, J. Stevenson, C.-Q. Sun, E. W. Petrillo, D. S. Karanewski, M. M. Asaad, J. E. Bird, T. R. Schaeffer, N. C. Trippodo, Abstracts of papers, 210th Am. Chem. Soc Meeting, Chicago, Ill., MEDI 064 (1995).

Templates (k): See D. BenIshai, A. R. McMurray, Tetrahedron 1993, 49, 6399.

Templates (l): See E. G. von Roedern, H. Kessler, Angew. Chem. Int. Ed. Engl. 1994, 33, 687–689.

Templates (m): See R. Gonzalez-Muniz, M. J. Dominguez, M. T. Garcia-Lopez, Tetrahedron 1992, 48, 5191–5198.

Templates (n): See F. Esser, A. Carpy, H. Briem, H. KΓΆppen, K.-H. Pook, Int. J. Pept. Res. 1995, 45, 540–546.

Templates (o): See N. De la Figuera, I. Alkorta, T. Garcia-Lopez, R. Herranz, R. Gonzalez-Muniz, Tetrahedron 1995, 51, 7841.

Templates (p): See U. Slomcynska, D. K. Chalmers, F. Cornille, M. L. Smythe, D. D. Benson, K. D. Moeller, G. R. Marshall, J. Org. Chem. 1996, 61, 1198–1204.

The Ξ²-hairpin peptidomimetics of the invention can be used in a wide range of applications in order to inhibit the growth of or to kill microorganisms and/or cancer cells.

They can be used for example as disinfectants or as preservatives for materials such as foodstuffs, cosmetics, medicaments and other nutrient-containing materials or for preventing surfaces from microbial colonization [J. M. Schierholz, C. Fleck, J. Beuth, G. Pulverer, J. Antimicrob. Chemother., 2000, 46, 45–50]. The Ξ²-hairpin peptidomimetics of the invention can also be used to treat or prevent diseases related to microbial infection in plants and animals.

For use as disinfectants or preservatives the Ξ²-hairpin peptidomimetics can be added to the desired material singly, as mixtures of several Ξ²-hairpin peptidomimetics or in combination with other antimicrobial agents. The Ξ²-hairpin peptidomimetics may be administered per se or may be applied as an appropriate formulation together with carriers, diluents or excipients well known in the art, expediently in a form suitable for oral, topical, transdermal, injection, buccal, transmucosal, pulmonary or inhalation administration, such as tablets, dragees, capsules, solutions, liquids, gels, plasters, creams, ointments, syrups, slurries, suspensions, sprays, nebulisers or suppositories.

When used to treat or prevent infections or diseases related to such infections or cancer, the Ξ²-hairpin peptidomimetics can be administered singly, as mixtures of several Ξ²-hairpin peptidomimetics, in combination with other antimicrobial, antibiotic or anicancer agents or in combination with other pharmaceutically active agents. The Ξ²-hairpin peptidomimetics can be administered per se or as pharmaceutical compositions.

Pharmaceutical compositions comprising Ξ²-hairpin peptidomimetics of the invention may be manufactured by means of conventional mixing, dissolving, granulating, coated tablet-making, levigating, emulsifying, encapsulating, entrapping or lyophilizing processes. Pharmaceutical compositions may be formulated in conventional manner using one or more physiologically acceptable carriers, diluents, excipients or auxilliaries which facilitate processing of the active Ξ²-hairpin peptidomimetics into preparations which can be used pharmaceutically. Proper formulation depends upon the method of administration chosen.

For topical administration the Ξ²-hairpin peptidomimetics of the invention may be formulated as solutions, gels, ointments, creams, suspensions, etc. as are well-known in the art.

Systemic formulations include those designed for administration by injection, e.g. subcutaneous, intravenous, intramuscular, intrathecal or intraperitoneal injection, as well as those designed for transdermal, transmucosal, oral or pulmonary administration.

For injections, the Ξ²-hairpin peptidomimetics of the invention may be formulated in adequate solutions, preferably in physiologically compatible buffers such as Hink's solution, Ringer's solution, or physiological saline buffer. The solution may contain formulatory agents such as suspending, stabilizing and/or dispersing agents. Alternatively, the Ξ²-hairpin peptidomimetics of the invention may be in powder form for combination with a suitable vehicle, e.g., sterile pyrogen-free water, before use.

For transmucosal administration, penetrants appropriate to the barrier to be permeated are used in the formulation as known in the art.

For oral administration, the compounds can be readily formulated by combining the active Ξ²-hairpin peptidomimetics of the invention with pharmaceutically acceptable carriers well known in the art. Such carriers enable the Ξ²-hairpin peptidomimetics of the invention to be formulated as tablets, pills, dragees, capsules, liquids, gels, syrups, slurries, suspensions etc., for oral ingestion of a patient to be treated. For oral formulations such as, for example, powders, capsules and tablets, suitable excipients include fillers such as sugars, such as lactose, sucrose, mannitol and sorbitol; cellulose preparations such as maize starch, wheat starch, rice starch, potato starch, gelatin, gum tragacanth, methyl cellulose, hydroxypropylmethyl cellulose, sodium carboxymethylcellulose, and/or polyvinylpyrrolidone (PVP); granulating agents; and binding agents. If desired, desintegrating agents may be added, such as cross-linked polyvinylpyrrolidones, agar, or alginic acid or a salt thereof, such as sodium alginate. If desired, solid dosage forms may be sugar-coated or enteric-coated using standard techniques.

For oral liquid preparations such as, for example, suspensions, elixirs and solutions, suitable carriers, excipients or diluents include water, glycols, oils, alcohols, etc. In addition, flavoring agents, preservatives, coloring agents and the like may be added.

For buccal administration, the composition may take the form of tablets, lozenges, etc. formulated as usual.

For administration by inhalation, the Ξ²-hairpin peptidomimetics of the invention are conveniently delivered in form of an aeorosol spray from pressurized packs or a nebulizer, with the use of a suitable propellant, e.g. dichlorodifluoromethane, trichlorofluromethane, carbon dioxide or another suitable gas. In the case of a pressurized aerosol the dose unit may be determined by providing a valve to deliver a metered amount Capsules and cartridges of e.g. gelatin for use in an inhaler or insufflator may be formulated containing a powder mix of the Ξ²-hairpin peptidomimetics of the invention and a suitable powder base such as lactose or starch.

The compounds may also be formulated in rectal or vaginal compositions such as suppositories together with appropriate suppository bases such as cocoa butter or other glycerides.

In addition to the formulation described previously, the Ξ²-hairpin peptidomimetics of the invention may also be formulated as depot preparations. Such long acting formulations may be administered by implantation (e.g. subcutaneously or intramuscularly) or by intramuscular injection. For the manufacture of such depot preparations the Ξ²-hairpin peptidomimetics of the invention may be formulated with suitable polymeric or hydrophobic materials (e.g. as an emulsion in an acceptable oil) or ion exchange resins, or as sparingly soluble salts.

In addition, other pharmaceutical delivery systems may be employed such as liposomes and emulsions well known in the art. Certain organic solvents such as dimethylsulfoxide also may be employed. Additionally, the Ξ²-hairpin peptidomimetics of the invention may be delivered using a sustained-release system, such as semipermeable matrices of solid polymers containing the therapeutic agent. Various sustained-release materials have been established and are well known by those skilled in the art. Sustained-release capsules may, depending on their chemical nature, release the compounds for a few weeks up to over 100 days. Depending on the chemical nature and the biological stability of the therapeutic agent, additional strategies for protein stabilization may be employed.

As the Ξ²-hairpin pepdidomimetics of the invention may contain charged residues, they may be included in any of the above-described formulations as free bases or as pharmaceutically acceptable salts. Pharmaceutically acceptable salts tend to be more soluble in aqueous and other protic solvents than are the corresponding free base forms.

The Ξ²-hairpin peptidomimetics of the invention, or compositions thereof, will generally be used in an amount effective to achieve the intended purpose. It is to be understood that the amount used will depend on a particular application.

For example, for use as a desinfectant or preservative, an antimicrobially effective amount of a Ξ²-hairpin peptidomimetic of the invention, or a composition thereof, is applied or added to the material to be desinfected or preserved. By antimicrobially effective amount is meant an amount of a Ξ²-hairpin peptidomimetic of the invention or composition that inhibits the growth of, or is lethal to, a target microbe population. While the antimicrobially effective amount will depend on a particular application, for use as desinfectants or preservatives the Ξ²-hairpin peptidomimetics of the invention, or compositions thereof, are usually added or applied to the material to be desinfected or preserved in relatively low amounts. Typically, the Ξ²-hairpin peptidomimetics of the invention comprise less than about 5% by weight of a desinfectant solution or material to be preserved, preferably less than 1% by weight and more preferably less than 0.1% by weight. An ordinary skilled expert will be able to determine antimicrobially effective amounts of particular Ξ²-hairpin pepdidomimetics of the invention for particular applications without undue experimentation using, for example, the in vitro assays provided in the examples.

For use to treat or prevent microbial infections or diseases related thereto and cancer, the Ξ²-hairpin pepidomimetics of the invention, or compositions thereof, are administered or applied in a therapeutically effective amount. By therapeutically effective amount is meant an amount effective in ameliorating the symptoms of, or ameliorate, treat or prevent microbial infections or diseases related thereto. Determination of a therapeutically effective amount is well within the capacities of those skilled in the art, especially in view of the detailed disclosure provided herein.

As in the case of desinfectants and preservatives, for topical administration to treat or prevent bacterial, yeast, fungal or other infections a therapeutically effective dose can be determined using, for example, the in vitro assays provided in the examples. The treatment may be applied while the infection is visible, or even when it is not visible. An ordinary skilled expert will be able to determine therapeutically effective amounts to treat topical infections without undue experimentation.

For systemic administration, a therapeutically effective dose can be estimated initially from in vitro assays. For example, a dose can be formulated in animal models to achieve a circulating Ξ²-hairpin peptidomimetic concentration range that includes the IC50 as determined in the cell culture (i.e. the concentration of a test compound that is lethal to 50% of a cell culture), the MIC, as determined in cell culture (i.e. the concentration of a test compound that is lethal to 100% of a cell culture). Such information can be used to more accurately determine useful doses in humans.

Initial dosages can also be determined from in vivo data, e.g. animal models, using techniques that are well known in the art. One having ordinary skills in the art could readily optimize administration to humans based on animal data.

Dosage amount for applications as antimicrobial agents may be adjusted individually to provide plasma levels of the Ξ²-hairpin peptidomimetics of the invention which are sufficient to maintain the therapeutic effect. Usual patient dosages for administration by injection range from about 0.1–5 mg/kg/day, preferably from about 0.5 to 1 mg/kg/day. Therapeutically effective serum levels may be achieved by administering multiple doses each day.

In cases of local administration or selective uptake, the effective local concentration of the Ξ²-hairpin peptidomimetics of the invention may not be related to plasma concentration. One having the skills in the art will be able to optimize therapeutically effective local dosages without undue experimentation.

The amount of Ξ²-hairpin peptidomimetics administered will, of course, be dependent on the subject being treated, on the subject's weight, the severity of the affliction, the manner of administration and the judgement of the prescribing physician.

The antimicrobial therapy may be repeated intermittently while infections are detectable or even when they are not detectable. The therapy may be provided alone or in combination with other drugs, such as for example antibiotics or other antimicrobial agents.

Normally, a therapeutically effective dose of the Ξ²-hairpin peptidomimetics described herein will provide therapeutic benefit without causing substantial toxicity.

Hemolysis of red blood cells is often employed for assessment of toxicity of related compounds such as protegrin or tachyplesin. Values are given as %-lysis of red blood cells observed at a concentration of 100 ΞΌg/ml. Typical values determined for cationic peptides such as protegrin and tachyplesin range between 30–40% with average MIC-values of 1–5 ΞΌg/ml over a wide range of pathogens. Normally, Ξ²-hairpin peptidomimetics of the invention will show hemolysis in a range of 0.5–10%, often in a range of 1–5%, at activity levels comparable to those mentioned above for protegrin and tachyplesin. Thus preferred compounds exhibit low MIC-values and low %-hemolysis of red blood cells observed at a concentration of 100 ΞΌg/ml.

Toxicity of the Ξ²-hairpin peptidomimetics of the invention herein can be determined by standard pharmaceutical procedures in cell cultures or experimental animals, e.g., by determining the LD50 (the dose lethal to 50% of the population) or the LD100 (the dose lethal to 100% of the population). The dose ratio between toxic and therapeutic effect is the therapeutic index. Compounds which exhibit high therapeutic indices are preferred. The data obtained from these cell culture assays and animal studies can be used in formulating a dosage range that is not toxic for use in humans. The dosage of the Ξ²-hairpin peptidomimetics of the invention lies preferably within a range of circulating concentrations that include the effective dose with little or no toxicity. The dosage may vary within the range depending upon the dosage form employed and the route of administration utilized. The exact formulation, route of administration and dose can be chosen by the individual physician in view of the patient's condition (see, e.g. Fingl et at. 1975, In: The Pharmacological Basis of Therapeutics, Ch. 1, p. 1).

The following Examples illustrate the invention in more detail but are not intended to limit its scope in any way. The following abbreviations are used in these Examples:

  • HBTU: 1-benzotriazol-1-yl-tetramethylurounium hexafluorophosphate (Knorr et al. Tetrahedron Lett. 1989, 30, 1927–1930)
  • HOBt: 1-hydroxybenzotriazole
  • DIEA: diisopropylethylamine
  • HOAT: 7-aza-1-hydroxybenzotriazole
  • HATU: O-(7-aza-benzotriazole-1-yl)-N,N,Nβ€²,Nβ€²-tetramethyluronoium hexafluorophosphate Carpino et al. Tetrahedron Lett. 1994, 35, 2279–2281)

EXAMPLES

1. Peptide Synthesis

Coupling of the First Protected Amino Acid Residue

0.5 g of 2-chlorotritylchloride resin (Barlos et al. Tetrahedron Lett. 1989, 30, 3943–3946) (0.83 mMol/g, 0.415 mmol) was filled into a dried flask The resin was suspended in CH2Cl2 (2.5 ml) and allowed to swell at room temperature under constant stirring. The resin was treated with 0.415 mMol (1 eq) of the first suitably protected amino acid residue (see below) and 284 ΞΌl (4 eq) of diisopropylethylamine (IDEA) in CH2Cl2 (2.5 ml), the mixture was shaken at 25Β° C. for 15 minutes, poured onto the pre-swollen resin and stirred at 25Β° C. for 18 hours. The resin colour changed to purple and the solution remained yellowish. The resin was washed extensively (CH2Cl2/MeOH/DIEA: 17/2/1; CH2Cl2, DMF; CH2Cl2; Et2O, 3 times each) and dried under vacuum for 6 hours.

Loading was typically 0.6–0.7 mMol/g.

The following preloaded resins were prepared: Fmoc-GlyO-chlorotritylresin; Fmoc-Arg(Pbf)O-chlorotritylresin; Fmoc-Lys(Boc)O-chlorotritylresin.

1.1. Procedure 1

The synthesis was carried out using a Syro-peptide synthesizer (Multisyntech) using 24 to 96 reaction vessels. In each vessel was placed 60 mg (weight of the resin before loading) of the above resin. The following reaction cycles were programmed and carried out:

Step Reagent Time
1 CH2Cl2, wash and swell (manual)  3 Γ— 1 min.
2 DMF, wash and swell  1 Γ— 5 min.
3 40% piperidine/DMF  1 Γ— 5 min.
4 DMF, wash  5 Γ— 2 min.
5 5 equiv. Fmoc amino acid/DMF + 1 Γ— 120 min.
5 eq. HBTU + 5 eq. HOBt + 5 eq. DIEA
6 DMF, wash  4 Γ— 2 min.
7 CH2Cl2, wash (at the end of the synthesis)  3 Γ— 2 min.

Steps 3 to 6 are repeated to add each amino-acid.

Cleavage of the Fully Protected Peptide Fragment

After completion of the synthesis, the resin was suspended in 1 ml (0.39 mMol) of 1% TFA in CH2Cl2 (v/v) for 3 minutes, filtered and the filtrate was neutralized with 1 ml (1.17 mMol, 3 eq.) of 20% DIEA in CH2Cl2 (v/v). This procedure was repeated twice to ensure completion of the cleavage. The filtrate was evaporated to dryness and the product was fully deprotected to be analyzed by reverse phase-HPLC (column C18) to monitor the efficiency of the linear peptide synthesis.

Cyclization of the Linear Peptide

100 mg of the fully protected linear peptide were dissolved in DMF (9 ml, conc. 10 mg/ml). Then 41.8 mg (0.110 mMol, 3 eq.) of HATU, 14.9 mg (0.110 mMol, 3 eq) of HOAt and 1 ml (0.584 mMol) of 10% DIEA in DMF (v/v) were added and the mixture vortexed at 20Β° C. for 16 hours and subsequently concentrated under high vacuum. The residue was partitioned between CH2Cl2 and H2O/CH3CN (90/10: v/v). The CH2Cl2 phase was evaporated to yield the fully protected cyclic peptide.

Deprotection and Purification of the Cyclic Peptide

The cyclic peptide obtained was dissolved in 1 ml of the cleavage mixture containing 95% trifluoroacetic acid (TFA), 2.5% water and 2.5% triisopropylsilane (TIS). The mixture was left to stand at 20Β° C. for 2.5 hours and then concentrated under vacuum. The residue was dissolved in a solution of H2O/acetic acid (75/25: v/v) and the mixture extracted with di-isopropylether.

The water phase was dried under vacuum and then the product purified by preparative reverse phase HPLC.

After lyophilisation products were obtained as a white powder and analysed by ESI-MS. The analytical data comprising HPLC retension times and ESI-MS are shown in tables 1–7. Analytical HPLC retension times (RT, in minutes) were determined using a VYDAC 218TP104 (length 25 cm) column with gradient A: (10% CH3CN+0.1% TFA and 90% H2O+0.1% TFA to 98% CH3CN+0.1% TFA and 2% H2O+0.1% TFA in 20 minutes) and with gradient B: (10% CH3CN+0.1% TFA and 90% H2O+0.1% TFA to 98% CH3CN+0.1% TFA and 2% H2O+0.1% TFA in 21 minutes).

Examples ex.1–7 (n=8) are shown in table 1. The peptides were synthesized starting with the amino acid at position P4 which was coupled to the resin. Starting resins were Fmoc-Arg(Pbf)O-chlorotritylresin and Fmoc-Lys(Boc)O-chlorotritylresin, which were prepared as described above. The linear peptides were synthesized on solid support according to procedure 1 in the following sequence: P5-P6-P7-P8-DPro-P1-P2-P3-P4-resin, cleaved, cyclized, deprotected and purified as indicated. HPLC-retension times (minutes) were determined using gradient A.

Examples ex.831 (n=9) are shown in table 2. The peptides were synthesized starting with the amino acid at position P5 which was coupled to the resin. Starting resin was Fmoc-Arg(Pbf)O-chlorotritylresin, which was prepared as described above. The linear peptides were synthesized on solid support according to procedure 1 in the following sequence: P6-P7-P8-P9-DPro-Pro-P1-P2-P3-P4-P5-resin, cleaved, cyclized, deprotected and purified as indicated. HPLC-retension times (minutes) were determined using gradient A.

Examples ex.32–58 (n=10) are shown in table 3. The peptides were synthesized staring with the amino acid at position P5 which was coupled to the resin. Starting resin was Fmoc-Arg(Pbf)O-chlorotr;tykesin, which was prepared as described above. The linear peptides were synthesized on solid support according to procedure 1 in the following sequence: P6-P7-P8-P9-P10-DPro-Pro-P1-P2-P3-P4-P5-resin, cleaved, cyclized, deprotected and purified as indicated. HPLC-retension times (minutes) were determined using gradient A.

Examples ex.59–70 (n=11) are shown in table 4. The peptides were synthesized starting with the amino acid at position P5 which was coupled to the resin. Starting resin was Fmoc-Arg(Pbf)O-chlorotritylresin, which was prepared as described above. The linear peptides were synthesized on solid support according to procedure 1 in the following sequence: P6-P7-P8-P9-P10-P11-DPro-Pro-P1-P2-P3-P4-P5-resin, cleaved, cyclized, deprotected and purified as indicated. HPLC-retension times (minutes) were determined using gradient A.

Examples ex.71–84 (n=14) are shown in table 5. The peptides were synthesized starting with the amino acid at position P7 which was coupled to the resin. Starting resin was Fmoc-Arg(Pbf)O-chlorotritylresin, which was prepared as described above. The linear peptides were synthesized on solid support according to procedure 1 in the following sequence: P8-P9-P10-P11-P12-P13-P14-DPro-P1-P2-P3-P4-P5-P6-P7-resin, cleaved, cyclized, deprotected and purified as indicated. HPLC-retension times (minutes) were determined using gradient A.

Examples ex.85–95 (n=16) are shown in table 6. The peptides were synthesized staring with the amino acid at position P8 which was coupled to the resin. Starting resins were Fmoc-Arg(Pbf)O-chlorotritylresin and Fmoc-Lys(Boc)O-chlorotritylresin, which were prepared as described above. The linear peptides were synthesized on solid support according to procedure 1 in the following sequence: P9-P10-P11-P12-P13-P13-P15-P16-DPro-P1-P2-P3-P4-P5-P6-P7-P8-resin, cleaved, cyclized, deprotected and purified as indicated. HPLC-retension times (minutes) were determined using gradient A.

Examples ex.96–246, ex.276 (n=12) are shown in table 7. The peptides (exept ex.177 and ex.181) were synthesized starting with the amino acid at position P6 which was grafted to the resin. Starting resins were Fmoc-Arg(Pbf)O-chlorotritylresin and Fmoc-Lys(Boc)O-chlorotritylresin, which were prepared as described above. The linear peptides were synthesized on solid support according to procedure 1 in the following sequence: P7-P8-P9-P10-P11-P12-DPro-Pro-P1-P2-P3-P4-P5-P6-resin, cleaved, cyclized, deprotected and purified as indicated. HPLC-retension times (minutes) were determined using gradient A.

Examples ex.177 to ex.181 (n=12) are shown in table 7. The peptides were synthesized starting with the amino acid at position P7 which was coupled to the resin. Starting resin was Fmoc-Arg(Pbf)O-chlorotritylresin, which were prepared as described above. The linear peptides were synthesized on solid support according to procedure 1 in the following sequence: P8-P9-P10-P11-P12-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, cleaved, cyclized, deprotected and purified as indicated HPLC-retension times (minutes) were determined using gradient A.

Examples ex.247–277 (n=12) are shown in table 7. The peptides were synthesized starting with the amino acid at position P6 which was grafted to the resin. Starting resins were Fmoc-Arg(Pbf)O-chlorotritylesin and Fmoc-Lys(Boc)O-chlorotritylresin, which were prepared as described above. The linear peptides were synthesized on solid support according to procedure 1 in the following sequence: P7-P8-P9-P10-P11-P12-DPro-BB-P1-P2-P3-P4-P5-P6-resin, cleaved, cyclized, deprotected and purified as indicated.

BB: Gly (ex.247); Arg(Pmc) (ex.248); Y (Bzl) (ex.249); Phe (ex250); Trp (ex.251); Leu (ex.252); Ile (ex.253); Cha (ex.254); 2-Nal (ex.255); 219a (ex.256); 219b (ex.257); 219c (ex.258); 219d (ex.259); 219e (ex.260); 219f (ex.261); 219g (ex.262); 219h (ex.263); 219i (ex.264); 219k (ex.265); 219l (ex.266); 219m (ex267); 219n (ex.268); 219o (ex.269); 219p (ex.270); 219q (ex.271); 219r (ex.272); 219s (ex.273); 219t (ex.274), 219u (ex.275).

Building blocks 219a–u are described below.

Example ex.277 (n=12) is shown in table 7. The peptide was synthesized starting with the amino acid at position P6 which was grafted to the resin. Starting resin was Fmoc-Arg(Pbf)O-chlorotritylresin, which were prepared as described above. The linear peptide was synthesized on solid support according to procedure 1 in the following sequence: P7-P5-P9-P10-P11-P12-(c1-1)-P1-P2-P3-P4-P5-P6-resin, cleaved, cyclized, deprotected and purified as indicated.

Building block (c1-1) is described below.

Examples ex.278–300 (n=12) are shown in table 7. The peptides were synthesized starting with the amino acid at position P6 which was grafted to the resin. Starting resins were Fmoc-Arg(Pbf)O-chlorotritylresin, Fmoc-Tyr(Bzl)O-chlorotrityl resin and Fmoc-)Tyr(Bzl)O-chlorotrityl resin which were prepared as described above. The linear peptide was synthesized on solid support according to procedure 1 in the following sequence: P7-P8-P9-P10-P11-P12-DPro-Pro-P1-P2-P3-P4-P5-P6-resin, cleaved, cyclized, deprotected and purified as indicated. Analytical HPLC-retention times (RT, in minutes) were determined using a VYDAC 218TP104 (length 25 cm) column with gradient B (10% CH3CN+0.1% TFA and 90% H2O+0.1% TFA to 98% CH3CN+0.1% TFA and 2% H2O+0.1% TFA in 21 minutes).

Retention times (minutes) were the following: ex.278 (11.43); ex.279 (11.64); ex.280 (10.57); ex.281 (10.04); ex282 (10.63); ex.283 (10.00); ex.284 (9.21).

Retention times (minutes) for examples 285–300 were determined with gradient C: VYDAC C18-column (length 15 cm); (8% CH3CN+0.1% TFA and 92% H2O+0.1% TFA to 62.8% CH3CN+0.1% TFA and 37.2% H2O+0.1% TFA in 8 minutes to 100% CH3CN+0.1% TFA in 9 minutes).

ex.285 (5.37; 5.57)*; ex.286 (5.17); ex.287 (5.0); ex.288 (4.15;4.37)*; ex.289 (4.47; 4.72)*; ex.290 (3.45; 3.72)*; ex.291 (3.65; 3.82)*; ex.292 (4.27); ex.293 (4.10); ex.294 (3.83; 4.13)*; ex.296 (4.38; 4.67)*; ex.297 (4.10; 4.32)*; ex.298 (4.12); ex.299 (4.47); ex.300 (5.03). * double peaks which show both correct MS and chiral amino acid analysis. At 60Β° only one peak is observed.

TABLE 1
Examples ex. 1–7 (n = 8)
Example SEQ. ID P1 P2 P3 P4 P5 P6 P7 P8 Template RT(β€²) %a) MS
1. SEQ ID NO: 1 Tyr Val Arg Arg Arg Phe Leu Val DProLPro 18.6 76 1284.6
2. SEQ ID NO: 2 Tyr Val Arg Lys Gly Phe Leu Val DProLPro 18.8 86 1157.4
3. SEQ ID NO: 3 Trp Val Arg Lys Gly Phe Leu Trp DProLPro 22.0 70 1263.8
4. SEQ ID NO: 4 Tyr Val Arg Arg Arg Trp Leu Val DProLPro 19.1 35 1323.6
5. SEQ ID NO: 5 Tyr Val Tyr Arg Arg Phe Leu Val DProLPro 20.7 81 1287.6
6. SEQ ID NO: 6 Lys Val Tyr Arg Arg Phe Leu Val DProLPro 16.7 75 1256.6
7. SEQ ID NO: 7 Lys Val Tyr Lys Gly Phe Leu Trp DProLPro 19.5 64 1216.5
a)%-purity of crude product. All compounds were purified by preparative HPLC-chromatography as indicated. Purities > 90%.

TABLE 2
Examples ex. 8–29 (n = 9)
Example SEQ. ID P1 P2 P3 P4 P5 P6 P7 P8 P9 Template RT(β€²) %a) MS
8. SEQ ID NO: 8 Arg Phe Leu Arg Arg Arg Leu Phe Arg DProLPro 10.5 35 1495.9
9. SEQ ID NO: 9 Arg Tyr Leu Arg Arg Arg Leu Tyr Arg DProLPro 8.8 46 1527.9
10. SEQ ID NO: 10 Arg Phe Phe Arg Arg Arg Leu Phe Arg DProLPro 10.0 26 1529.9
11. SEQ ID NO: 11 Arg Tyr Tyr Arg Arg Arg Leu Tyr Arg DProLPro 8.0 90 1577.9
12. SEQ ID NO: 12 Leu Phe Phe Arg Arg Arg Leu Phe Arg DProLPro 10.2 52 1502.9
13. SEQ ID NO: 13 Leu Tyr Tyr Arg Arg Arg Leu Tyr Arg DProLPro 8.4 30 1550.9
14. SEQ ID NO: 14 Arg Phe Leu Phe Arg Arg Leu Leu Arg DProLPro 10.1 51 1468.9
15. SEQ ID NO: 15 Arg Tyr Leu Tyr Arg Arg Leu Leu Arg DProLPro 8.8 55 1500.9
16. SEQ ID NO: 16 Leu Phe Leu Phe Arg Arg Leu Phe Arg DProLPro 9.7 38 1459.9
17. SEQ ID NO: 17 Leu Tyr Leu Tyr Arg Arg Leu Tyr Arg DProLPro 11.8 67 1507.9
18. SEQ ID NO: 18 Arg Phe Leu Phe Arg Arg Leu Phe Leu DProLPro 10.3 57 1459.9
19. SEQ ID NO: 19 Arg Tyr Leu Tyr Arg Arg Leu Tyr Leu DProLPro 11.7 66 1507.9
20. SEQ ID NO: 20 Phe Leu Leu Phe Arg Arg Leu Phe Arg DProLPro 9.9 67 1459.9
21. SEQ ID NO: 21 Tyr Leu Leu Tyr Arg Arg Leu Tyr Arg DProLPro 11.9 57 1507.9
22. SEQ ID NO: 22 Arg Leu Leu Phe Arg Arg Leu Phe Phe DProLPro 10.1 68 1459.9
23. SEQ ID NO: 23 Arg Leu Leu Tyr Arg Arg Leu Tyr Tyr DProLPro 11.5 63 1507.9
24. SEQ ID NO: 24 Arg Phe Leu Arg Arg Phe Leu Phe Arg DProLPro 8.5 33 1502.9
25. SEQ ID NO: 25 Arg Phe Leu Arg Arg Phe Phe Leu Arg DProLPro 10.3 30 1502.9
26. SEQ ID NO: 26 Arg Tyr Leu Arg Arg Tyr Tyr Leu Arg DProLPro 12.6 65 1550.9
27. SEQ ID NO: 27 Leu Tyr Leu Arg Arg Tyr Leu Tyr Arg DProLPro 10.1 29 1491.8
28. SEQ ID NO: 28 Leu Leu Phe Phe Arg Arg Leu Phe Arg DProLPro 12.1 35 1443.8
29. SEQ ID NO: 29 Leu Leu Tyr Tyr Arg Arg Leu Tyr Arg DProLPro 10.3 33 1491.8
30. SEQ ID NO: 30 Arg Leu Phe Phe Arg Arg Leu Phe Leu DProLPro 12.1 35 1459.9
31. SEQ ID NO: 31 Arg Leu Tyr Tyr Arg Arg Leu Tyr Leu DProLPro 10.3 33 1507.8
a)%-purity of crude product. All compounds were purified by preparative HPLC-chromatography as indicated. Purities obtained > 90%.

TABLE 3
Examples ex. 32–58 (n = 10)
Example Sequ. ID P1 P2 P3 P4 P5 P6 P7 P8 P9 P10 Template RT(β€²) %a) MS
32. SEQ ID NO: 32 Arg Phe Leu Phe Arg Arg Arg Leu Phe Arg DProLPro 10.2 37 1643.0
33. SEQ ID NO: 33 Arg Tyr Leu Tyr Arg Arg Arg Leu Tyr Arg DProLPro 8.3 41 1691.0
34. SEQ ID NO: 34 Arg Phe Phe Phe Arg Arg Arg Leu Leu Arg DProLPro 10.1 45 1643.0
35. SEQ ID NO: 35 Arg Tyr Tyr Tyr Arg Arg Arg Leu Leu Arg DProLPro 8.87 70 1691.0
36. SEQ ID NO: 36 Arg Leu Phe Phe Arg Arg Arg Leu Phe Arg DProLPro 10.4 56 1643.0
37. SEQ ID NO: 37 Leu Tyr Leu Tyr Arg Arg Arg Leu Tyr Arg DProLPro 9.6 35 1648.0
38. SEQ ID NO: 38 Arg Phe Leu Phe Arg Arg Arg Leu Phe Leu DProLPro 11.1 50 1600.0
39. SEQ ID NO: 39 Arg Tyr Leu Tyr Arg Arg Arg Leu Tyr Leu DProLPro 9.81 41 1648.0
40. SEQ ID NO: 40 Leu Leu Phe Phe Arg Arg Arg Leu Phe Arg DProLPro 11.8 58 1600.0
41. SEQ ID NO: 41 Arg Leu Phe Phe Arg Arg Arg Leu Phe Leu DProLPro 11.6 54 1600.0
42. SEQ ID NO: 42 Leu Tyr Tyr Tyr Arg Arg Arg Leu Leu Arg DProLPro 9.9 51 1648.0
43. SEQ ID NO: 43 Arg Phe Phe Phe Arg Arg Arg Leu Leu Leu DProLPro 11.3 49 1600.0
44. SEQ ID NO: 44 Arg Tyr Tyr Tyr Arg Arg Arg Leu Leu Leu DProLPro 9.9 63 1648.0
45. SEQ ID NO: 45 Arg Leu Leu Phe Arg Gly Arg Phe Phe Arg DProLPro 10.6 78 1543.9
46. SEQ ID NO: 46 Arg Leu Leu Tyr Arg Gly Arg Tyr Tyr Arg DProLPro 9.1 45 1591.9
47. SEQ ID NO: 47 Arg Phe Phe Phe Arg Gly Arg Leu Leu Arg DProLPro 10.4 43 1543.9
48. SEQ ID NO: 48 Arg Tyr Tyr Tyr Arg Gly Arg Leu Leu Arg DProLPro 8.8 48 1591.9
49. SEQ ID NO: 49 Leu Phe Leu Phe Arg Gly Arg Leu Phe Arg DProLPro 12.4 65 1500.9
50. SEQ ID NO: 50 Leu Tyr Leu Tyr Arg Gly Arg Leu Tyr Arg DProLPro 10.3 58 1548.9
51. SEQ ID NO: 51 Arg Phe Leu Phe Arg Gly Arg Leu Phe Leu DProLPro 12.3 42 1500.9
52. SEQ ID NO: 52 Arg Tyr Leu Tyr Arg Gly Arg Leu Tyr Leu DProLPro 10.6 20 1548.9
53. SEQ ID NO: 53 Leu Arg Phe Phe Arg Leu Arg Leu Phe Arg DProLPro 11.9 51 1600.0
54. SEQ ID NO: 54 Leu Arg Tyr Tyr Arg Leu Arg Leu Tyr Arg DProLPro 9.9 50 1648.0
55. SEQ ID NO: 55 Leu Leu Phe Phe Arg Gly Arg Leu Phe Arg DProLPro 12.5 50 1500.9
56. SEQ ID NO: 56 Leu Leu Tyr Tyr Arg Gly Arg Leu Tyr Arg DProLPro 10.1 38 1548.9
57. SEQ ID NO: 57 Arg Phe Leu Phe Arg Gly Arg Phe Arg Leu DProLPro 11.3 57 1543.9
58. SEQ ID NO: 58 Arg Tyr Leu Tyr Arg Gly Arg Tyr Arg Leu DProLPro 10.8 56 1591.9
a)%-purity of crude product. All compounds were purified by preparative HPLC-chromatography as indicated. Purities obtained > 90%.

TABLE 4
Examples ex. 59–70 (n = 11)
Ex-
am-
ple SEQ. ID P1 P2 P3 P4 P5 P6 P7 P8 P9 P10 P11 Template RT(β€²) % MS
59. SEQ ID NO: 59 Arg Leu Phe Leu Arg Arg Arg Phe Phe Arg Leu DProLPro 11.1 75 1756.2
60. SEQ ID NO: 60 Arg Leu Tyr Leu Arg Arg Arg Tyr Tyr Arg Leu DProLPro 9.5 28 1804.2
61. SEQ ID NO: 61 Leu Leu Phe Leu Arg Arg Arg Phe Phe Arg Arg DProLPro 10.8 65 1756.2
62. SEQ ID NO: 62 Arg Leu Phe Leu Arg Arg Arg Leu Phe Arg Phe DProLPro 11.3 57 1756.2
63. SEQ ID NO: 63 Phe Leu Phe Leu Arg Arg Arg Leu Phe Arg Arg DProLPro 11.1 76 1756.2
64. SEQ ID NO: 64 Tyr Leu Tyr Leu Arg Arg Arg Leu Tyr Arg Arg DProLPro 9.5 70 1804.2
65. SEQ ID NO: 65 Arg Arg Phe Leu Arg Gly Arg Phe Phe Leu Arg DProLPro 9.8 36 1700.1
66. SEQ ID NO: 66 Leu Leu Tyr Tyr Arg Arg Leu Tyr Tyr Arg Arg DProLPro 9.9 47 1811.2
67. SEQ ID NO: 67 Leu Tyr Leu Tyr Arg Arg Tyr Leu Tyr Arg Arg DProLPro 9.9 47 1811.2
68. SEQ ID NO: 68 Arg Arg Phe Phe Arg Arg Leu Phe Phe Leu Leu DProLPro 12.4 46 1747.2
69. SEQ ID NO: 69 Arg Leu Tyr Tyr Arg Arg Leu Tyr Tyr Arg Leu DProLPro 9.9 51 1811.2
70. SEQ ID NO: 70 Arg Leu Phe Phe Arg Gly Arg Phe Phe Arg Leu DProLPro 10.5 26 1691.1
a)%-purity of crude product. All compounds were purified by preparative HPLC-chromatography as indicated. Purities > 90%.

TABLE 5
Examples ex. 71–84 (n = 14)
Example SEQ. ID P1 P2 P3 P4 P5 P6 P7 P8 P9 P10
71. SEQ ID NO: 71 Arg Tyr Leu Leu Tyr Arg Arg Arg Tyr Leu
72. SEQ ID NO: 72 Arg Leu Leu Tyr Tyr Arg Arg Arg Tyr Leu
73. SEQ ID NO: 73 Arg Leu Leu Leu Tyr Arg Arg Arg Tyr Leu
74. SEQ ID NO: 74 Arg Phe Leu Phe Leu Arg Arg Arg Phe Phe
75. SEQ ID NO: 75 Arg Tyr Leu Tyr Leu Arg Arg Arg Tyr Tyr
76. SEQ ID NO: 76 Arg Phe Leu Phe Leu Arg Arg Arg Phe Leu
77. SEQ ID NO: 77 Arg Tyr Leu Tyr Leu Arg Arg Arg Tyr Leu
78. SEQ ID NO: 78 Arg Arg Leu Leu Phe Arg Arg Arg Phe Leu
79. SEQ ID NO: 79 Arg Arg Leu Leu Tyr Arg Arg Arg Tyr Leu
80. SEQ ID NO: 80 Arg Arg Leu Tyr Tyr Arg Arg Arg Tyr Leu
81. SEQ ID NO: 81 Arg Arg Leu Leu Tyr Arg Arg Arg Tyr Leu
82. SEQ ID NO: 82 Arg Arg Leu Phe Leu Arg Arg Arg Phe Phe
83. SEQ ID NO: 83 Arg Arg Leu Tyr Leu Arg Arg Arg Tyr Tyr
84. SEQ ID NO: 84 Arg Arg Leu Tyr Leu Arg Arg Arg Tyr Leu
Example SEQ. ID P11 P12 P13 P14 Template RT(β€²) % MS
71. SEQ ID NO: 71 Leu Tyr Arg Arg DProLPro 9.4 48 2236.7
72. SEQ ID NO: 72 Leu Tyr Arg Arg DProLPro 9.4 29 2236.7
73. SEQ ID NO: 73 Tyr Tyr Arg Arg DProLPro 9.4 50 2236.7
74. SEQ ID NO: 74 Leu Phe Arg Arg DProLPro 10.9 78 2206.7
75. SEQ ID NO: 75 Leu Tyr Arg Arg DProLPro 9.1 51 2286.7
76. SEQ ID NO: 76 Phe Leu Arg Arg DProLPro 10.6 79 2172.7
77. SEQ ID NO: 77 Tyr Leu Arg Arg DProLPro 9.1 53 2236.7
78. SEQ ID NO: 78 Leu Phe Phe Arg DProLPro 11.0 42 2172.7
79. SEQ ID NO: 79 Leu Tyr Tyr Arg DProLPro 9.4 91 2236.7
80. SEQ ID NO: 80 Leu Tyr Tyr Arg DProLPro 9.3 72 2286.7
81. SEQ ID NO: 81 Tyr Tyr Leu Arg DProLPro 9.5 65 2236.7
82. SEQ ID NO: 82 Leu Phe Phe Arg DProLPro 11.1 34 2206.7
83. SEQ ID NO: 83 Leu Tyr Tyr Arg DProLPro 9.3 89 2286.7
84. SEQ ID NO: 84 Tyr Leu Tyr Arg DProLPro 9.3 47 2236.7
a)%-purity of crude product. All compounds were purified by preparative HPLC-chromatography. Purities > 90%.

TABLE 6
Examples ex. 85–95 (n = 16)
Example Sequ. ID P1 P2 P3 P4 P5 P6 P7 P8 P9 P10 P11
85. SEQ ID NO: 85 Lys Arg Leu Lys Tyr Val Arg Arg Arg Trp Leu
86. SEQ ID NO: 86 Lys Arg Leu Lys Tyr Val Arg Arg Gly Trp Leu
87. SEQ ID NO: 87 Lys Arg Leu Lys Tyr Trp Arg Arg Arg Trp Tyr
88. SEQ ID NO: 88 Lys Arg Leu Tyr Tyr Trp Arg Arg Arg Trp Tyr
89. SEQ ID NO: 89 Lys Arg Leu Lys Tyr Trp Arg Arg Gly Trp Tyr
90. SEQ ID NO: 90 Lys Arg Leu Tyr Tyr Trp Arg Arg Gly Trp Tyr
91. SEQ ID NO: 91 Lys Arg Leu Tyr Tyr Trp Arg Arg Arg Trp Lys
92. SEQ ID NO: 92 Lys Arg Leu Lys Tyr Trp Arg Arg Gly Trp Lys
93. SEQ ID NO: 93 Tyr Lys Leu Arg Leu Lys Tyr Arg Arg Trp Lys
94. SEQ ID NO: 94 Tyr Lys Leu Gln Leu Lys Trp Arg Arg Phe Lys
95. SEQ ID NO: 95 Tyr Lys Leu Gln Leu Gln Lys Lys Gly Trp Gln
Example Sequ. ID P12 P13 P14 P15 P16 Template RT(β€²) % MS
85. SEQ ID NO: 85 Val Lys Val Leu Arg DProLPro 13.7 70 2346.0
86. SEQ ID NO: 86 Val Lys Val Leu Arg DProLPro 13.9 38 2246.8
87. SEQ ID NO: 87 Val Lys Val Leu Arg DProLPro 13.6 34 2483.1
88. SEQ ID NO: 88 Val Phe Val Leu Arg DProLPro 14.3 35 2537.1
89. SEQ ID NO: 89 Val Lys Val Leu Arg DProLPro 13.7 27 2383.9
90. SEQ ID NO: 90 Val Phe Val Leu Arg DProLPro 14.6 39 2437.9
91. SEQ ID NO: 91 Val Phe Val Leu Arg DProLPro 13.9 22 2402.1
92. SEQ ID NO: 92 Val Lys Val Leu Arg DProLPro 13.4 26 2348.9
93. SEQ ID NO: 93 Tyr Arg Val Lys Phe DProLPro 12.5 34 2402.1
94. SEQ ID NO: 94 Tyr Gln Val Lys Phe DProLPro 12.1 21 2348.9
95. SEQ ID NO: 95 Tyr Gln Val Lys Phe DProLPro 11.1 84 2383.9
a)%-purity of crude product. All compounds were purified by preparative HPLC-chromatography. Purities > 90%.

TABLE 7
Example Sequ. ID P1 P2 P3 P4 P5 P6 P7 P8 P9 P10 P11 P12 Template RT(β€²) % MS
Examples ex. 96–128 (n = 12);
96. SEQ ID NO: 96 Leu Arg Leu Val Tyr Lys Gly Phe Leu Tyr Arg Val DProLPro 21.6 92 1703.1
97. SEQ ID NO: 97 Leu Arg Phe Val Tyr Lys Gly Phe Leu Tyr Arg Val DProLPro 21.6 95 1737.1
98. SEQ ID NO: 98 Leu Arg Thr Val Tyr Lys Gly Phe Leu Tyr Arg Val DProLPro 20.0 93 1691.1
99. SEQ ID NO: 99 Leu Arg Lys Val Arg Lys Gly Arg Leu Tyr Arg Val DProLPro 15.7 99 1720.2
100. SEQ ID NO: 100 Leu Arg Lys Trp Tyr Lys Gly Phe Trp Tyr Arg Val DProLPro 17.6 60 1878.3
101. SEQ ID NO: 101 Leu Arg Lys Val Tyr Arg Gly Phe Leu Tyr Arg Val DProLPro 17.8 61 1845.3
102. SEQ ID NO: 102 Leu Lys Lys Val Tyr Arg Arg Phe Leu Lys Lys Val DProLPro 15.9 59 1754.3
103. SEQ ID NO: 103 Leu Arg Leu Lys Tyr Arg Arg Phe Lys Tyr Arg Val DProLPro 20.5 36 1874.3
104. SEQ ID NO: 104 Leu Arg Leu Glu Tyr Arg Arg Phe Glu Tyr Arg Val DProLPro 21.5 99 1876.2
105. SEQ ID NO: 105 Leu Arg Leu Gln Tyr Arg Arg Phe Gln Tyr Arg Val DProLPro 21.5 58 1874.2
106. SEQ ID NO: 106 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 18.1 51 1879.7
107. SEQ ID NO: 107 Leu Arg Leu Lys Trp Arg Arg Lys Lys Tyr Arg Val DProLPro 20.2 28 1879.7
108. SEQ ID NO: 108 Leu Arg Trp Lys Tyr Arg Arg Phe Lys Tyr Arg Val DProLPro 20.9 40 1948.7
109. SEQ ID NO: 109 Lys Val Arg Phe Arg Arg Arg Lys Leu Lys Leu Arg DProLPro 15.7 75 1833.7
110. SEQ ID NO: 110 Leu Arg Leu Gln Tyr Arg Arg Trp Gln Tyr Arg Val DProLPro 21.9 30 1913.3
111. SEQ ID NO: 111 Leu Arg Leu Gln Trp Arg Arg Phe Gln Tyr Arg Val DProLPro 22.6 75 1897.3
112. SEQ ID NO: 112 Leu Arg Leu Gln Lys Arg Arg Trp Gln Tyr Arg Val DProLPro 18.9 49 1878.3
113. SEQ ID NO: 113 Leu Arg Leu Gln Trp Arg Arg Lys Gln Tyr Arg Val DProLPro 21.2 75 1878.3
114. SEQ ID NO: 114 Phe Arg Leu Gln Tyr Arg Arg Phe Gln Tyr Arg Val DProLPro 22.3 50 1908.3
115. SEQ ID NO: 115 Leu Arg Leu Gln Tyr Arg Arg Phe Gln Tyr Arg Phe DProLPro 22.4 99 1908.3
116. SEQ ID NO: 116 Phe Arg Leu Gln Tyr Arg Arg Phe Gln Tyr Arg Phe DProLPro 22.9 99 1956.3
117. SEQ ID NO: 117 Leu Arg Leu Gln Tyr Arg Arg Phe Gln Trp Arg Val DProLPro 22.7 15 1897.3
118. SEQ ID NO: 118 Leu Arg Trp Gln Tyr Arg Arg Phe Gln Tyr Arg Val DProLPro 21.9 21 1947.3
119. SEQ ID NO: 119 Gln Val Arg Phe Arg Arg Arg Lys Leu Gln Leu Arg DProLPro 17.2 46 1831.3
120. SEQ ID NO: 120 Phe Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.5 52 1912.4
121. SEQ ID NO: 121 Cha Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.6 36 1918.4
122. SEQ ID NO: 122 hPhe Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 9.6 95 1926.4
123. SEQ ID NO: 123 2Nal Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 9.6 69 1962.4
124. SEQ ID NO: 124 1Nal Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 11.8 47 1962.4
125. SEQ ID NO: 125 Nle Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.3 63 1878.4
126. SEQ ID NO: 126 Leu Arg Phe Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.6 44 1912.4
127. SEQ ID NO: 127 Leu Arg Cha Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.8 41 1918.4
128. SEQ ID NO: 128 Leu Arg Y(bzl) Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 11.5 23 2018.5
Examples ex. 129–161 (n = 12)
129. SEQ ID NO: 129 Leu Arg Trp Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.5 41 1951.4
130. SEQ ID NO: 130 Leu Arg hPhe Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.6 32 1926.4
131. SEQ ID NO: 131 Leu Arg 2Nal Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 11.0 42 1962.4
132. SEQ ID NO: 132 Leu Arg 1Nal Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.9 43 1962.4
133. SEQ ID NO: 133 Leu Arg Val Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.0 47 1864.3
134. SEQ ID NO: 134 Leu Arg Ile Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.3 34 1878.4
135. SEQ ID NO: 135 Leu Arg Nle Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.3 90 1878.4
136. SEQ ID NO: 136 Leu Arg Leu Lys Lys Arg Arg Tyr Lys Tyr Arg Val DProLPro 9.9 48 1855.3
137. SEQ ID NO: 137 Leu Arg Leu Lys Lys Arg Arg Y(Bzl) Lys Tyr Arg Val DProLPro 11.0 33 1945.4
138. SEQ ID NO: 138 Leu Arg Leu Lys Lys Arg Arg hPhe Lys Tyr Arg Val DProLPro 10.3 52 1853.3
139. SEQ ID NO: 139 Leu Arg Leu Lys Lys Arg Arg 2Nal Lys Tyr Arg Val DProLPro 10.5 53 1889.4
140. SEQ ID NO: 140 Leu Arg Leu Lys Lys Arg Arg 1Nal Lys Tyr Arg Val DProLPro 10.5 34 1889.4
141. SEQ ID NO: 141 Leu Arg Leu Lys Lys Arg Arg Val Lys Tyr Arg Val DProLPro 9.9 49 1889.4
142. SEQ ID NO: 142 Leu Arg Leu Lys Lys Arg Arg Ile Lys Tyr Arg Val DProLPro 10.0 32 1791.3
143. SEQ ID NO: 143 Leu Arg Leu Lys Lys Arg Arg Leu Lys Tyr Arg Val DProLPro 10.1 46 1805.3
144. SEQ ID NO: 144 Leu Arg Leu Lys Lys Arg Arg Nle Lys Tyr Arg Val DProLPro 10.1 43 1805.3
145. SEQ ID NO: 145 Leu Arg Leu Lys Lys Arg Arg His Lys Tyr Arg Val DProLPro 9.8 56 1829.3
146. SEQ ID NO: 146 Leu Arg Leu Lys Lys Arg Arg Trp Lys Phe Arg Val DProLPro 10.9 45 1862.3
147. SEQ ID NO: 147 Leu Arg Leu Lys Lys Arg Arg Trp Lys Y(Bzl) Arg Val DProLPro 11.4 15 1968.5
148. SEQ ID NO: 148 Leu Arg Leu Lys Lys Arg Arg Trp Lys Trp Arg Val DProLPro 10.8 56 1901.4
149. SEQ ID NO: 149 Leu Arg Leu Lys Lys Arg Arg Trp Lys hPhe Arg Val DProLPro 11.3 32 1876.4
150. SEQ ID NO: 150 Leu Arg Leu Lys Lys Arg Arg Trp Lys 1Nal Arg Val DProLPro 11.6 24 1912.4
151. SEQ ID NO: 151 Leu Arg Leu Lys Lys Arg Arg Trp Lys Val Arg Val DProLPro 10.6 48 1814.3
152. SEQ ID NO: 152 Leu Arg Leu Lys Lys Arg Arg Trp Lys Ile Arg Val DProLPro 10.9 40 1828.3
153. SEQ ID NO: 153 Leu Arg Leu Lys Lys Arg Arg Trp Lys Leu Arg Val DProLPro 10.7 18 1828.3
154. SEQ ID NO: 154 Leu Arg Leu Lys Lys Arg Arg Trp Lys Nle Arg Val DProLPro 11.2 40 1828.3
155. SEQ ID NO: 155 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Phe DProLPro 10.6 35 1926.4
156. SEQ ID NO: 156 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Cha DProLPro 11.2 60 1932.5
157. SEQ ID NO: 157 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Y(Bzl) DProLPro 11.7 37 2032.5
158. SEQ ID NO: 158 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Trp DProLPro 10.4 69 1965.4
159. SEQ ID NO: 159 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg hPhe DProLPro 10.8 95 1940.4
160. SEQ ID NO: 160 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg 2Nal DProLPro 11.2 30 1976.5
161. SEQ ID NO: 161 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg 1Nal DProLPro 11.3 89 1976.5
Examples ex. 162–194 (n = 12)
162. SEQ ID NO: 162 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Ile DProLPro 10.5 56 1892.4
163. SEQ ID NO: 163 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Nle DProLPro 10.5 91 1892.4
164. SEQ ID NO: 164 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg His DProLPro 8.6 88 1916.4
165. SEQ ID NO: 165 Leu Trp Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.4 55 1908.4
166. SEQ ID NO: 166 Leu Leu Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.6 88 1835.3
167. SEQ ID NO: 167 Leu Thr Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.4 94 1823.3
168. SEQ ID NO: 168 Leu Gln Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.4 55 1850.3
169. SEQ ID NO: 169 Leu Arg Leu Leu Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.9 62 1863.3
170. SEQ ID NO: 170 Leu Arg Leu Arg Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.3 45 1906.4
171. SEQ ID NO: 171 Leu Arg Leu Thr Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.4 94 1851.3
172. SEQ ID NO: 172 Leu Arg Leu Gln Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.3 76 1878.3
173. SEQ ID NO: 173 Leu Arg Leu Lys Leu Arg Arg Trp Lys Tyr Arg Val DProLPro 11.9 43 1863.3
174. SEQ ID NO: 174 Leu Arg Leu Lys His Arg Arg Trp Lys Tyr Arg Val DProLPro 10.5 53 1887.3
175. SEQ ID NO: 175 Leu Arg Leu Lys Arg Arg Arg Trp Lys Tyr Arg Val DProLPro 10.4 37 1906.4
176. SEQ ID NO: 176 Leu Arg Leu Lys Thr Arg Arg Trp Lys Tyr Arg Val DProLPro 11.4 45 1851.3
177. SEQ ID NO: 177 Leu Arg Leu Lys Lys Leu Arg Trp Lys Tyr Arg Val DProLPro 10.8 58 1835.3
178. SEQ ID NO: 178 Leu Arg Leu Lys Lys His Arg Trp Lys Tyr Arg Val DProLPro 10.2 46 1859.3
179. SEQ ID NO: 179 Leu Arg Leu Lys Lys Lys Arg Trp Lys Tyr Arg Val DProLPro 10.3 53 1850.3
180. SEQ ID NO: 180 Leu Arg Leu Lys Lys Thr Arg Trp Lys Tyr Arg Val DProLPro 10.4 82 1823.3
181. SEQ ID NO: 181 Leu Arg Leu Lys Lys Gln Arg Trp Lys Tyr Arg Val DProLPro 10.4 36 1850.3
182. SEQ ID NO: 182 Leu Arg Leu Lys Lys Arg Trp Trp Lys Tyr Arg Val DProLPro 10.8 70 1908.4
183. SEQ ID NO: 183 Leu Arg Leu Lys Lys Arg His Trp Lys Tyr Arg Val DProLPro 10.3 74 1859.3
184. SEQ ID NO: 184 Leu Arg Leu Lys Lys Arg Lys Trp Lys Tyr Arg Val DProLPro 10.2 50 1850.3
185. SEQ ID NO: 185 Bip Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 11.4 39 1988.5
186. SEQ ID NO: 186 4ClPhe Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 11.1 53 1946.8
187. SEQ ID NO: 187 AmPhe Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 8.6 83 1927.4
188. SEQ ID NO: 188 S(Bzl) Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.4 66 1942.4
189. SEQ ID NO: 189 T(Bzl) Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.8 51 1956.4
190. SEQ ID NO: 190 Orn Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 8.4 84 1879.3
191. SEQ ID NO: 191 Leu Arg Bip Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 11.3 39 1988.5
192. SEQ ID NO: 192 Leu Arg 4ClPhe Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.9 50 1946.8
193. SEQ ID NO: 193 Leu Arg AmPhe Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 9.2 82 1927.4
194. SEQ ID NO: 194 Leu Arg S(Bzl) Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.7 80 1942.4
Examples ex. 195–227 (n = 12)
195. SEQ ID NO: 195 Leu Arg T(Bzl) Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.7 37 1956.4
196. SEQ ID NO: 196 Leu Arg Orn Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 9.2 48 1879.3
197. SEQ ID NO: 197 Leu Arg Leu Lys Lys Arg Arg Bip Lys Tyr Arg Val DProLPro 10.8 57 1915.4
198. SEQ ID NO: 198 Leu Arg Leu Lys Lys Arg Arg 4ClPhe Lys Tyr Arg Val DProLPro 10.4 49 1873.8
199. SEQ ID NO: 199 Leu Arg Leu Lys Lys Arg Arg AmPhe Lys Tyr Arg Val DProLPro 9.8 43 1854.3
200. SEQ ID NO: 200 Leu Arg Leu Lys Lys Arg Arg S(Bzl) Lys Tyr Arg Val DProLPro 10.3 48 1869.3
201. SEQ ID NO: 201 Leu Arg Leu Lys Lys Arg Arg T(Bzl) Lys Tyr Arg Val DProLPro 10.2 87 1883.4
202. SEQ ID NO: 202 Leu Arg Leu Lys Lys Arg Arg Orn Lys Tyr Arg Val DProLPro 9.7 31 1806.3
203. SEQ ID NO: 203 Leu Arg Leu Lys Lys Arg Arg Trp Lys Bip Arg Val DProLPro 11.6 46 1938.5
204. SEQ ID NO: 204 Leu Arg Leu Lys Lys Arg Arg Trp Lys 4ClPhe Arg Val DProLPro 11.21 48 1896.8
205. SEQ ID NO: 205 Leu Arg Leu Lys Lys Arg Arg Trp Lys S(Bzl) Arg Val DProLPro 11.5 32 1892.4
206. SEQ ID NO: 206 Leu Arg Leu Lys Lys Arg Arg Trp Lys T(Bzl) Arg Val DProLPro 11.5 36 1906.4
207. SEQ ID NO: 207 Leu Arg Leu Lys Lys Arg Arg Trp Lys Orn Arg Val DProLPro 9.4 49 1829.3
208. SEQ ID NO: 208 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Bip DProLPro 11.7 37 2002.5
209. SEQ ID NO: 209 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg 4ClPhe DProLPro 11.0 32 1960.8
210. SEQ ID NO: 210 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg AmPhe DProLPro 8.6 88 1941.4
211. SEQ ID NO: 211 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg T(Bzl) DProLPro 10.9 51 1970.5
212. SEQ ID NO: 212 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Orn DProLPro 8.3 75 1893.4
213. SEQ ID NO: 213 Leu Orn Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.3 63 1836.3
214. SEQ ID NO: 214 Leu Arg Leu Orn Lys Arg Arg Trp Lys Tyr Arg Val DProLPro 10.4 44 1864.3
215. SEQ ID NO: 215 Leu Arg Leu Lys Orn Arg Arg Trp Lys Tyr Arg Val DProLPro 10.2 44 1864.3
216. SEQ ID NO: 216 Leu Arg Leu Lys Lys Arg Orn Trp Lys Tyr Arg Val DProLPro 10.2 44 1836.3
217. SEQ ID NO: 217 Leu Arg Leu Lys Lys Arg Arg Trp Orn Tyr Arg Val DProLPro 10.3 40 1864.3
218. SEQ ID NO: 218 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Orn Val DProLPro 10.2 92 1836.3
219. SEQ ID NO: 219 Leu Arg Leu Lys Lys Arg Gln Trp Lys Tyr Arg Val DProLPro 10.4 92 1850.3
220. SEQ ID NO: 220 Leu Arg Leu Lys Lys Arg Arg Trp Tyr Tyr Arg Val DProLPro 10.5 88 1913.4
221. SEQ ID NO: 221 Leu Arg Leu Lys Lys Arg Arg Trp His Tyr Arg Val DProLPro 10.4 49 1887.3
222. SEQ ID NO: 222 Leu Arg Leu Lys Lys Arg Arg Trp Arg Tyr Arg Val DProLPro 10.3 53 1906.4
223. SEQ ID NO: 223 Leu Arg Leu Lys Lys Arg Arg Trp Thr Tyr Arg Val DProLPro 10.5 84 1851.3
224. SEQ ID NO: 224 Leu Arg Leu Lys Lys Arg Arg Trp Gln Tyr Arg Val DProLPro 10.5 52 1878.3
225. SEQ ID NO: 225 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Val DProLPro 10.6 54 1885.3
226. SEQ ID NO: 226 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Trp Val DProLPro 10.9 47 1908.4
227. SEQ ID NO: 227 Leu Arg Leu Lys Lys Arg Arg Bip Lys Bip Arg Val DProLPro 12.3 50 1975.5
Examples ex. 228–255 (n = 12)
228. SEQ ID NO: 228 Leu Arg Leu Arg Lys Arg Arg Bip Lys Tyr Arg Val DProLPro 10.9 46 1943.4
229. SEQ ID NO: 229 Leu Arg Leu Lys Lys Arg Arg Bip Arg Tyr Arg Val DProLPro 10.9 41 1943.4
230. SEQ ID NO: 230 Leu Trp Leu Lys Lys Arg Arg Bip Lys Tyr Arg Val DProLPro 11.0 73 1945.4
231. SEQ ID NO: 231 Leu Trp Leu Arg Lys Arg Arg Bip Lys Tyr Arg Val DProLPro 11.0 71 1973.5
232. SEQ ID NO: 232 Leu Trp Leu Lys Lys Arg Arg Bip Arg Tyr Arg Val DProLPro 11.0 71 1973.5
233. SEQ ID NO: 233 Leu Trp Leu Arg Lys Arg Arg Bip Lys Bip Arg Val DProLPro 12.4 60 2033.6
234. SEQ ID NO: 234 Leu Trp Leu Lys Lys Arg Arg Bip Arg Bip Arg Val DProLPro 12.4 85 2033.6
235. SEQ ID NO: 235 Leu Trp Leu Arg Lys Arg Arg Bip Arg Bip Arg Bip DProLPro 11.6 50 2185.7
236. SEQ ID NO: 236 4ClPhe Arg Leu Lys Lys Arg Arg Bip Lys Tyr Arg Val DProLPro 10.7 39 1983.9
237. SEQ ID NO: 237 4ClPhe Arg Leu Lys Lys Arg Arg Bip Lys Bip Arg Val DProLPro 13.0 36 2043.9
238. SEQ ID NO: 238 4ClPhe Arg Leu Lys Lys Arg Arg Bip Lys Tyr Arg Bip DProLPro 12.9 52 2108.0
239. SEQ ID NO: 239 4ClPhe Arg Leu Lys Lys Arg Arg Bip Lys Bip Arg Bip DProLPro 12.6 68 2168.1
240. SEQ ID NO: 240 4ClPhe Arg Leu Arg Lys Arg Arg Bip Lys Tyr Arg Val DProLPro 11.7 46 2011.9
241. SEQ ID NO: 241 4ClPhe Arg Leu Lys Lys Arg Arg Bip Arg Tyr Arg Val DProLPro 11.7 41 2011.9
242. SEQ ID NO: 242 4ClPhe Trp Leu Lys Lys Arg Arg Bip Lys Tyr Arg Val DProLPro 11.8 48 2013.9
243. SEQ ID NO: 243 4ClPhe Trp Leu Arg Lys Arg Arg Bip Lys Tyr Arg Val DProLPro 11.9 38 2041.9
244. SEQ ID NO: 244 4ClPhe Trp Leu Lys Lys Arg Arg Bip Arg Tyr Arg Val DProLPro 11.9 74 2041.9
245. SEQ ID NO: 245 4ClPhe Trp Leu Arg Lys Arg Arg Bip Lys Bip Arg Val DProLPro 13.2 66 2102.0
246. SEQ ID NO: 246 4ClPhe Trp Leu Lys Lys Arg Arg Bip Arg Bip Arg Val DProLPro 13.2 49 2102.0
247. SEQ ID NO: 247 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-Gly 9.5 58 1838.3
248. SEQ ID NO: 248 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-Arg 9.3 57 1937.4
249. SEQ ID NO: 249 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-Tyr 9.9 29 1944.4
250. SEQ ID NO: 250 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-Phe 10.7 34 1928.4
251. SEQ ID NO: 251 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-Trp 10.7 25 1967.5
252. SEQ ID NO: 252 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-Leu 10.5 21 1894.4
253. SEQ ID NO: 253 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-Ile 10.4 42 1894.4
254. SEQ ID NO: 254 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-Cha 11.2 36 1934.5
255. SEQ ID NO: 255 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-2Nal 11.4 27 1978.5
Examples ex. 256–286 (n = 12)
All products were purified by preparative HPLC-chromatography. Purities > 90%.
Example Sequ. ID P1 P2 P3 P4 P5 P6 P7 P8 P9 P10 P11 P12 Template MS
256. SEQ ID NO: 256 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-1 1990.5
257. SEQ ID NO: 257 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-2 2018.3
258. SEQ ID NO: 258 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-3 2086.4
259. SEQ ID NO: 259 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-4 2086.4
260. SEQ ID NO: 260 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-5 1978.3
261. SEQ ID NO: 261 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-6 2023.3
262. SEQ ID NO: 262 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-7 1934.3
263. SEQ ID NO: 263 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-8 1948.2
264. SEQ ID NO: 264 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-9 1962.2
265. SEQ ID NO: 265 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-10 1976.3
266. SEQ ID NO: 266 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-11 1962.2
267. SEQ ID NO: 267 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-12 2002.3
268. SEQ ID NO: 268 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-13 2016.3
269. SEQ ID NO: 269 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-14 1976.3
270. SEQ ID NO: 270 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-15 1996.2
271. SEQ ID NO: 271 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-16 2011.4
272. SEQ ID NO: 272 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-17 2049.3
273. SEQ ID NO: 273 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-18 2063.4
274. SEQ ID NO: 274 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-19 2072.3
275. SEQ ID NO: 275 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val DPro-A8β€²-20 2046.4
276. SEQ ID NO: 276 Leu Arg Leu Lys Lys Gly Arg Trp Lys Tyr Arg Val DProLPro 1779.2
277. SEQ ID NO: 277 Leu Arg Leu Lys Lys Arg Arg Trp Lys Tyr Arg Val (c1)-1 2023.2
278. SEQ ID NO: 278 Leu Tyr Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Val DProLPro 1892.3
279. SEQ ID NO: 279 Leu Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Val DProLPro 1915.4
280. SEQ ID NO: 280 Arg Trp Leu Lys Lys Arg Arg Trp Lys Tyr Trp Val DProLPro 1981.4
281. SEQ ID NO: 281 Arg Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Val DProLPro 1958.4
282. SEQ ID NO: 282 Leu Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 1995.5
283. SEQ ID NO: 283 Leu Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 1972.4
284. SEQ ID NO: 284 Arg Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2015.5
285. SEQ ID NO: 285 Leu Arg Leu Lys Lys Y(Bzl) Arg Trp Lys Tyr Arg Val DProLPro 1975.5
286. SEQ ID NO: 286 Leu Arg Leu Lys Lys DY(Bzl) Arg Trp Lys Tyr Arg Val DProLPro 1975.5
Examples ex. 287–300 (n = 12)
All products were purified by preparative HPLC-chromatography. Purities > 90%.
287. SEQ ID NO: 287 Bip Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2082.6
288. SEQ ID NO: 288 Thr Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 1960.4
289. SEQ ID NO: 289 Arg Bip Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2052.5
290. SEQ ID NO: 290 Arg Thr Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 1930.4
291. SEQ ID NO: 291 Arg Trp Thr Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2003.4
292. SEQ ID NO: 292 Arg Trp Leu Arg Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2043.5
293. SEQ ID NO: 293 Arg Trp Leu Gln Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2015.4
294. SEQ ID NO: 294 Lys Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 1987.5
295. SEQ ID NO: 295 Tyr Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2022.5
296. SEQ ID NO: 296 Trp Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2045.5
297. SEQ ID NO: 297 Val Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2082.4
298. SEQ ID NO: 298 Gln Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 1987.4
299. SEQ ID NO: 299 Cha Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2012.5
300. SEQ ID NO: 300 Y Trp Leu Lys Lys Arg Arg Trp Lys Tyr Tyr Arg DProLPro 2112.6
(bzl)
a)%-purity of crude product. Purities of all compounds after prep. HPLC > 90%.

1.2. Procedure 2

Examples ex.256–275 were also synthesized using procedure 2.

The peptide synthesis was carried out by solid phase method using standard Fmoc chemistry on a peptide synthesizer-ABI 433A.

The first amino acid, Fmoc-Arg(Pbf)-OH (1.29 g, 1.2 equiv.) was coupled to the 2-chlorotritylchloride resin (Barlos et al. Tetrahedron Lett. 1989, 30, 3943–3946) (2 g, 0.83 mmol/g) in presence of DIEA (1.12 mL, 4 equiv.) in CH2Cl2 (20 mL), with swirling for 3 hr at room temperature. The resin was then washed with 3Γ—CH2Cl2/MeOH/DIEA(17:2:1), 3Γ—CH2Cl2, 2Γ—DMF, 2Γ—CH2Cl2, 2Γ—MeOH. Finally, the resin was dried under vacuum and the substitution level was measured by weight increase (˜0.6 mmol/g)

The resin with the synthesized linear peptide, Fmoc-Arg(Pbf)-Trp(Boc)-Lys(Boc)-Tyr(tBu)-Arg(Pbf)-Val-DPro-212-Leu-Arg(Pbf)-Leu-Lys(Boc)Lys(Boc)-Arg(Pbf)-resin, was preferably divided into equal parts and placed in different reaction vessels in order to carry out the acylation reaction in parallel format. The coupling and deprotection reactions in the following steps were monitored by Kaiser's test (Kaiser et al. Anal. Biochemistry 1970, 43, 595).

Removal of Alloc Protecting Group:

To the linear peptide resin (100 mg in each reaction vessel) was added Pd(PPh3)4 (15 mg, 0.5 equiv.) under argon followed by dry CH2Cl2 (10 mL) and phenylsilane (17 ΞΌL, 30 equiv.). The reaction mixture was left for 1 hour in the dark, filtered, and the resin was washed twice with CH2Cl2, DMF, and CH2Cl2.

Acylation of 4-amino-proline Group:

To the resin was added the corresponding acylating agent (usually a carboxyxlic acid (R64β€²COOH, 3 equiv.), HBTU (22.3 mg, 4 equiv.), HOBt (8 mg, 4 equiv.) and DIEA (125 ΞΌL, 6 equiv.) in DMF (2 mL) for 1.5–2 hrs at room temperature. The resin was filtered, washed with 2Γ—DMF, 3Γ—CH2Cl2, 2Γ—DMF.

Deprotection of NΞ±-Fmoc Group:

Deprotection of the Fmoc-group was achieved by treating the resin with 20% piperidine in DMF for 20 min. The resin was subsequently filtered and washed three times with DMF, and CH1Cl2, and twice with DMF, and CH2Cl2.

Cleavage of Peptide from the Resin:

The linear side-chain protected peptide was cleaved from the resin using AcOH:TFE:CH2Cl2 (2:2:6, v/v/v) for 2 hrs at room temperature. The resin was filtered off and washed twice with a mixture of AcOH:TFE:DCM and once with CH2Cl2. The filtrate was subsequently diluted with hexane (14 times by vol.) and concentrated. Evaporation was repeated twice with hexane to remove traces of AcOH. The residue was dried under vacuum. Yield of the linear protected peptide was generally about 40–50 mg.

Cyclization of the Linear Protected Peptide:

Cyclization was carried out in DMF at a concentration of 5 mg/mL using HATU (13.12 mg, 3 equiv.), HOAT (4.7 mg, 3 equiv.), DIEA (153 ΞΌL, 6 equiv.). The reaction mixture was stirred for 16 hrs at room temperature and the completion of reaction was monitored by HPLC. After the evaporation of DMF, CH3CN/H2O (90/10, v/v) was added to the residue and extracted with DCM. The organic layer was washed once with water and evaporated to dryness. Dried under vacuum.

Cleavage of Side Chain Protecting Groups:

The final deprotection of the side-chain protecting groups was carried out by treating the peptide with TFA:triisopropylsilane:H2O (95:2.5:2.5, v/v/v) at room temperature for 3 hrs. TFA was then evaporated and the residue triturated with cold ether.

Purification:

The crude peptides thus obtained were analyzed and purified by HPLC on a VYDAC C18 preparative column using 5–60% CH3CN/H2O+0.1% TFA in 30 min as gradient and a flow rate of 10 ml/min. The purity of the final peptide was checked by analytical HPLC and by ESI-MS. Analytical data are shown in table 7.

1.3. Procedure 3

Procedure 3 describes the synthesis of peptides having disulfide Ξ²-strand linkages.

a) n=8::The peptides are synthesized according to procedure 1 starting with the amino acid at position P4, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P5-P6-P7-P8-DPro-Pro-P1-P2-P3-P4-resin, where at positions P2 and P7 Fmoc-Cys(Acm)OH or Fmoc-hCys(Acm)OH are incorporated. The linear peptides are cleaved and cyclized as described in procedure 1. The cyclized side chain protected Ξ²-hairpin mimetics are dissolved in methanol (0.5 ml) to which is added dropwise a solution of iodine in methanol (1N, 1.5 equiv.) at room temperature. The reaction mixture is stirred for 4 hours at room temperature and the solvent evaporated. The crude product is subsequently deprotected and purified as described in procedure 1.

b) n=9::The peptides are synthesized according to procedure 1 starting with the amino acid at position P5, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P6-P7-P8-P9-DPro-Pro-P1-P2-P3-P4-P5-resin, where at positions P2 and P8 Fmoc-Cys(Acm)OH or Fmoc-hCys(Acm)OH are incorporated. The linear peptides are cleaved and cyclized as described in procedure 1. The cyclized side chain protected Ξ²-hairpin mimetics are dissolved in methanol (0.5 ml) to which is added dropwise a solution of iodine in methanol (1N, 1.5 equiv.) at room temperature. The reaction mixture is stirred for 4 hours at room temperature and the solvent evaporated. The crude product is subsequently deprotected and purified as described in procedure 1.

c) n=10::The peptides are synthesized according to procedure 1 starting with the amino acid at position P5, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P6-P7-P8-P9-P10-DPro-Pro-P1-P2-P3-P4-P5-resin, where at positions P3 and P8 Fmoc-Cys(Acm)OH or Fmoc-hCys(Acm)OH are incorporated. The linear peptides are cleaved and cyclized as described in procedure 1. The cyclized side chain protected Ξ²-hairpin mimetics are dissolved in methanol (0.5 ml) to which is added dropwise a solution of iodine in methanol (1N, 1.5 equiv.) at room temperature. The reaction mixture is stirred for 4 hours at room temperature and the solvent evaporated. The crude product is subsequently deprotected and purified as described in procedure 1.

d) n=11::The peptides are synthesized according to procedure 1 starting with the amino acid at position P5, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P6-P7-P8-P9-P10-P11-DPro-Pro-P1-P2-P3-P4-P5-resin, or P6-P7-P8-P9-P10-P11-DPro-Pro-P1-P2-P3-P4, or P5-P6-P7-P8-P9-P10-P11-DPro-Pro-P1-P2-P3-P4-P5-resin, where at positions P2, P4, P8 and P10 Fmoc-Cys(Acm)OH or Fmoc-hCys(Acm)OH are incorporated. The linear peptides are cleaved and cyclized as described in procedure 1. The cyclized side chain protected Ξ²-hairpin mimetics are dissolved in methanol (0.5 ml) to which is added dropwise a solution of iodine in methanol (1N, 1.5 equiv.) at room temperature. The reaction mixture is stirred for 4 hours at room temperature and the solvent evaporated. The crude product is subsequently deprotected and purified as described in procedure 1.

e) n=12::The peptides are synthesized according to procedure 1 starting with the amino acid at position P6, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence; P7-P8-P9-P10-P11-P12-DPro-Pro-P1-P2-P3-P4-P5-P6-resin, or P7-P8-P9-P10-P11-DPro-Pro-P1-P2-P3-P4-P5-P6-resin, or P7-P8-P9-P10-P11-DPro-Pro-P1-P2-P3-P4-P5-P6-resin, where at positions P2, P4, P9 and P11 Fmoc-Cys(Acm)OH or Fmoc-hCys(Acm)OH are incorporated. The linear peptides are cleaved and cyclized as described in procedure 1. The cyclized side chain protected Ξ²-hairpin mimetics are dissolved in methanol (0.5 ml) to which is added dropwise a solution of iodine in methanol (1N, 1.5 equiv.) at room temperature. The reaction mixture is stirred for 4 hours at room temperature and the solvent evaporated. The crude product is subsequently deprotected and purified as described in procedure 1.

Following procedure 3 NH2Arg(Pbf)-Lys(Boc)-Lys(Boc)-Cys(Acm)-Arg(Pbf)-Leu-Pro-DPro-Val-Arg-Cys(Acm)-Lys(Boc)-Trp(Boc)-Arg(Pbf)-[SEQ ID NO:301], coupled to the resin, was synthesized on the resin, the linear side-chain protected peptide cleaved and cyclized, followed by disulfide formation, deprotection and preparative HPLC chromatography yielding the above product [SEQ ID NO:302] as a white amorphous powder. ESI-MS: 1806.2 ([M+H]+).

  • f) n=14::The peptides are synthesized according to procedure 1 starting with the amino acid at position P7, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P8-P9-P10-P11-P12-P13-P14-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P8-P9-P10-P11-P12-P13-P14-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P8-P9-P10-P11-P12-P14-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, where at positions P3, P5, P10 and P12 Fmoc-Cys(Acm)OH or Fmoc-hCys(Acm)OH are incorporated. The linear peptides are cleaved and cyclized as described in procedure 1. The cyclized side chain protected Ξ²-hairpin mimetics are dissolved in methanol (0.5 ml) to which is added dropwise a solution of iodine in methanol (1N, 1.5 equiv.) at room temperature. The reaction mixture is stirred for 4 hours at room temperature and the solvent evaporated. The crude product is subsequently deprotected and purified as described in procedure 1.

g) n=16::The peptides are synthesized according to procedure 1 starting with the amino acid at position P8, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-P8-resin, or P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-P8-resin, or P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-P8-resin, or P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-P8-resin, or P9-P10-P11-P12-P13-P14-P51-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-P8-resin, or P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-P8-resin, or P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-P8-resin, where at positions P2, P4, P6, P11, P13 and P15 Fmoc-Cys(Acm)OH or Fmoc-hCys(Acm)OH are incorporated. The linear peptides are cleaved and cyclized as described in procedure 1. The cyclized side chain protected Ξ²-hairpin mimetics are dissolved in methanol (0.5 ml) to which is added dropwise a solution of iodine in methanol (1N, 1.5 equiv.) at room temperature. The reaction mixture is stirred for 4 hours at room temperature and the solvent evaporated. The crude product is subsequently deprotected and purified as described in procedure 1.

1.4. Procedure 4

Procedure 4 describes the synthesis of peptides having amide Ξ²-strand linkages.

a) n=8::The peptides are synthesized according to procedure 1 starting with the amino acid at position P4, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P5-P6-P7-P8-DPro-Pro-P1-P2-P3-P4-resin, where at position P2 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH, and at position P7 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH are incorporated. Alternatively, at position P2 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH, and at position P7 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH are incorporated. The linear peptides are cleaved and cyclized, and the alkyl groups are removed as described in procedure 2. The amide linkage is subsequently performed as described for the cyclization according to procedures 1 and 2, the side chain protective groups are removed and the products are purified as described in procedures 1 and 2.

b) nβ€”9::The peptides are synthesized according to procedure 1 starting with the amino acid at position P5, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P6-P7-P8-P9-DPro-Pro-P1-P2-P3-P4-P5-resin, where at position P2 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH, and at position P8 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH are incorporated. Alternatively, at position P2 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH, and at position P8 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH are incorporated. The linear peptides are cleaved and cyclized, and the alkyl groups are removed as described in procedure 2. The amide linkage is subsequently performed as described for the cyclization according to procedures 1 and 2, the side chain protective groups are removed and the products are purified as described in procedures 1 and 2.

c) n=10::The peptides are synthesized according to procedure 1 starting with the amino acid at position P5, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P6-P7-P5-P9-P10-DPro-Pro-P1-P2-P3-P4-P5-resin, where at position P3 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH, and at position P8 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH are incorporated. Alternatively, at position P3 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH, and at position P8 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH are incorporated. The linear peptides are cleaved and cyclized, and the alkyl groups are removed as described in procedure 2. The amide linkage is subsequently performed as described for the cyclization according to procedures 1 and 2, the side chain protective groups are removed and the products are purified as described in procedures 1 and 2.

d) n=11::The peptides are synthesized according to procedure 1 starting with the amino acid at position P5, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P6-P7-P8-P9-P10-P11-DPro-Pro-P1-P2-P3-P4-P5-resin, or P6-P7-P8-P9-P10-P11-DPro-Pro-P1-P2-P3-P4-P5-resin, or P6-P7-P8-P9-P10-P11-DPro-Pro-P1-P2-P3-P4-P5-resin; where at positions P2 and/or P4 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH, and at positions P8 and/or P10 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH are incorporated. Alternatively, at positions P2 and/or P4 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH, and at positions P8 and/or P10 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH are incorporated. The linear peptides are cleaved and cyclized, and the alkyl groups are removed as described in procedure 2. The amide linkage is subsequently performed as described for the cyclization according to procedures 1 and 2, the side chain protective groups are removed and the products are purified as described in procedures 1 and 2.

e) n=12::The peptides are synthesized according to procedure 1 starting with the amino acid at position P6, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P7-P8-P9-P10-P11-P12-DPro-Pro-P1-P2-P3-P4-P5-P6-resin, or P7-P8-P9-P10-P11-P12-DPro-Pro-P1-P2-P3-P4-P5-P6-resin, or P7-P8-P9-P10-P11-P12-DPro-Pro-P1-P2-P3-P4-P5-P6-resin; where at positions P2 and/or P4 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH, and at positions P9 and/or P11 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH are incorporated. Alternatively, at positions P2 and/or P4 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH, and at positions P9 and/or P11 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH are incorporated. The linear peptides are cleaved and cyclized, and the alkyl groups are removed as described in procedure 2. The amide linkage is subsequently performed as described for the cyclization according to procedures 1 and 2, the side chain protective groups are removed and the products are purified as described in procedures 1 and 2.

f) n=14::The peptides are synthesized according to procedure 1 starting with the amino acid at position P7, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P8-P9-P10-P11-P12-P3-P14-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P8-P9-P10-P11-P12-P13-P14-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P8-P9-P10-P11-P12-R14-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin; where at positions P3 and/or P5 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH, and at positions P10 and/or P12 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH are incorporated. Alternatively, at positions P3 and/or P5 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH, and at positions P10 and/or P12 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH are incorporated. The linear peptides are cleaved and cyclized, and the alkyl groups are removed as described in procedure 2. The amide linkage was subsequently performed as described for the cyclization according to procedures 1 and 2, the side chain protective groups are removed and the products are purified as described in procedures 1 and 2.

g) n=16::The peptides are synthesized according to procedure 1 starting with the amino acid at position P7, coupled to the resin. The linear peptides are synthesized on solid support according to procedure 1 in the following sequence: P8-P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P8-P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P9-P9-P10-P11-P12-P4-P5-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P8-P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P8-P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P8-P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin, or P8-P9-P10-P11-P12-P13-P14-P15-P16-DPro-Pro-P1-P2-P3-P4-P5-P6-P7-resin; where at positions P2 and/or P4 and/or P6 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH, and at positions P11 and/or P13 and/or P15 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH are incorporated. Alternatively, at positions P2 and/or P4 and/or P6 Fmoc-Orn(Alloc)OH or Fmoc-Lys(Alloc)OH, and at positions P11 and/or P13 and/or P15 Fmoc-Asp(OAllyl)OH or Fmoc-Glu(OAllyl)OH are incorporated. The linear peptides are cleaved and cyclized, and the alkyl groups are removed as described in procedure 2. The amide linkage is subsequently performed as described for the cyclization according to procedures 1 and 2, the side chain protective groups are removed and the products are purified as described in procedures 1 and 2.

Following procedure 2 NH2Arg(Pbf)-Trp(Boc)-Lys(Boc)-Tyr(tBu)-Arg(Pbf-DPro-212-Leu-Arg(Pbf)-Leu-Lys(Boc)-Lys(Boc)-Arg(Pbf)-[SEQ ID NO:303], coupled to the resin, was prepared, the linear peptide cleaved and cyclized. The Alloc-group was removed from building block 212 as described in procedure 2, half of the resulting amine reacted with excess glutaric anhydride in pyridine and DMAP and the solvents were removed. The resulting acid was coupled with the second half of the above mentioned amine in DMF and in the presence of TATU, HOAt and DIEA. The protective groups were removed as described in procedure 2 and the product purified by preparative HPLC chromatography as described in procedure 2 to yield the above product [SEQ ID NO:304] as a white amorphous powder. ESI-MS: 3882.3 ([M+H]+).

2. Synthesis of Templates

2.1. The synthesis of (2S,4S)-4-[(Allyloxy)carbonylamino]-1-[(9H-fluoren-9-yl)methoxycarbonyl]-proline (212) and (2S,4R)-4-[(Allyloxy)carbonylamino]-1-[(9H-fluoren-9-yl)methoxy-carbonyl]proline (217) are shown in Schemes 42 and 43.


(2S,4S)-4-[(Allyloxy)carbonylamino]-1-[(9H-fluoren-9-yl)methoxycarbonyl]-proline (212)

i,ii: To a solution of (2S,4R)-4-hydroxyproline (30 g, 0.18 mol) in abs. methanol (300 ml) at 0Β° C. thionyl chloride (38 ml, 2.5 eq, 0.45 mol) was added dropwise. The solution was heated to reflux and stirred for 3 h under nitrogen. Then the solution was concentrated by rotary evaporation and the ester precipitated by adding diethylether. After filtration the white solid was washed with diethylether, then dried at HV: (2S,4R)-4-hydroxyproline-methylester.hydrochloride as a white solid (29.9 g, 90%). %). TLC (CH2Cl2/MeOH/water 70:28:2): Rf 0.82. [Ξ±]D20=βˆ’24.5 (c=1.01, MeOH). IR (KBr): 3378s (br.), 2950m, 2863w, 1745s, 1700s, 1590 m, 1450s, 1415s, 1360s, 1215s, 1185s, 1080m, 700m. 1H-NMR (300 MHz, MeOH-d4) 4.66–4.55 (m, 2H, Hβ€”C(4), Hβ€”C(2)); 3.85 (s, 3H, H3β€”CO); 3.45 (dd, J=12.2, 3.8, 1H, Hβ€”C(5)); 3.37–3.25 (m, 1H, Hβ€”C(5)); 2.44–2.34 (m, 1H, Hβ€”C(3)), 2.27–2.12 (m, 1H, Hβ€”C(3)). 13C-NMR (75 MHz, MeOH-d4): 170.8 (s, COOMe); 70.8 (d, C(4)); 59.6 (d, C(2)); 55.2 (t, C(5)); 54.2 (q, Me); 38.7 (t, C(3)). CI-MS (NH3): 146.1 ([M-Cl]+).

30 g (0.17 mmol) of the above intermediate was dissolved in CH2Cl2 (300 ml), cooled to 0Β° C. and triethylamine (45 ml, 1.5 eq, 0.25 mol) was added dropwise. Then di-tert.-butyldicarbonate (54.0 g, 1.5 eq, 0.25 mmol) in CH1Cl2 (15 ml) and 4-N,N-dimethylaminopyridine (2.50 g, 0.1 eq, 17 mmol) was added and the solution stirred at room temperature overnight. Then the solution was washed with 1N aq. citric acid solution, sat. aq. NaHCO3 solution, dried (Na2SO4), evaporated and the residue dried at high vaccum: (2S,4R)-4-Hydroxy-1-[(tert-butoxy)carbonyl]proline-methylester (209) as a white solid (39.6 g, 78%). TLC (CH2Cl2/MeOH 9:1): Rf 0.55. [Ξ±]D24=βˆ’55.9 (c=0.983, CHCl3). IR (KBr): 3615w, 3440w (br.), 2980m, 2950m, 2880m, 1750s, 1705s, 1680s, 1480 m, 1410s, 1370s, 1340m, 1200s, 1160s, 1130m, 1090m, 1055w, 960w, 915w, 895w, 855m, 715m. 1H-NMR (300 MHz, CDCl3): 4.47–4.37 (m, 2H, Hβ€”C(4), Hβ€”C(2)); 3.73 (s, 3H, H3Cβ€”O)); 3.62 (dd, J=11.8, 4.1, 1H, Hβ€”C(5)); 3.54–3.44 (m, 1H, Hβ€”C(5)); 2.32–2.25 (m, 1H, Hβ€”C(3)); 2.10–2.03 (m, 1H, Hβ€”C(3)); 1.46+1.41 (2s, 9H, tBu). 13C-NMR (75 MHz, CDCl3): 173.6 (s, COOMe); 154.3+153.9 (2s, COOtBu); 80.3 (s, C-tBu); 70.0+69.3 (2d, C(4)); 57.9+57.4 (2d, C(2)); 54.6 (t, C(5)); 51.9 (q, Me); 39.0+38.4 (2t, C(3)); 28.1+27.6 (2q, tBu). CI-MS: 246.2 ([M+H]+); 190.1 ([M-tBu+H]+); 146.1 ([M-BOC+H]+).

iii,iv: 39 g (0.16 mol) of 209 was dissolved in CH2Cl2 (300 ml) followed by addition of 4-nitrobenzenesulfonyl chloride (46 g, 1.3 eq, 0.21 mol) and Et3N (33 ml, 1.5 eq, 0.24 mol) at 0Β° C. Then the solution was stirred overnight and brought gradually to room temperature, washed with 1N hydrochloric acid, sat. aq. NaHCO3 solution and dried (Na2SO4). The solvents were evaporated and the crude product was purified by filtration on silica gel with (2:1) hexane/AcOEt. The product was crystallized from hexane/AcOEt (2S,4S)-4-[(p-nitrobenzyl)sulfonyloxy]-1-[(tert-butoxy)carbonyl]proline methylester as white crystals (46.4 g, 65%). TLC (hexane/AcOEt 1:1): Rf 0.78. M.p.: 93–95Β° C. [Ξ±]D20=βˆ’32.3Β° (c=0.907, CHCl3). IR (KBr): 3110w, 3071w, 2971w, 1745s, 1696s, 1609s, 1532s, 1414s, 1365s, 1348m, 1289m, 1190m, 1173m, 1122w, 1097w, 1043w, 954w, 912w, 755w, 578w. 1H-NMR (600 MHz, CDCl3): 8.42–8.34 (m, 2H, H-C(Nos)); 8.11–8.04 (m, 2H, Hβ€”C(Nos)); 5.14 (s, 1H, Hβ€”C(4)); 4.39–4.28 (m, 1H, Hβ€”C(2)); 3.70–3.56 (m, 5H, H2β€”C(5), H3Cβ€”O); 2.58–2.38 (m, 1H, Hβ€”C(3)); 2.25–2.11 (m, 1H, Hβ€”C(3)); 1.37+1.33 (2s, 9H, tBu). 13C-NMR (150 MHz, CDCl3): 172.4+172.2 (2s, COOMe); 153.6+153.0 (2s, COOtBu); 150.8+142.0 (2s, C(Nos)); 129.0+124.6 (2d, C(Nos)); 80.4 (s, C-tBu); 80.8+79.9 (2d, C(4)); 57.1+56.9 (2d, C(2)); 52.2+51.7 (2t, C(5)); 52.3 (q, Me); 37.1+35.9 (2t, C(3)); 28.0 (q, tBu). ESI-MS (MeOH+NaI): 453.0 ([M+Na]+).

38 g (88 mmol) of the above intermediate was dissolved in DMF (450 ml) then heated to 40Β° C. when sodium azide (34 g, 6 eq, 0.53 mol) was added and the solution stirred overnight. DMF was evaporated and the solid suspended in diethylether. The suspension was washed with water and dried (Na2SO4). The solvent was evaporated and the product dried at high vacuum: (2S,4S)-4-Azido-1-[(tert-butoxy)carbonyl]proline methylester (210) yellow oil (21.1 g, 88%). [Ξ±]D20=βˆ’36.9 (c=0.965, CHCl3). 1H-NMR (600 MHz, CDCl3): 4.46–4.25 (2m, 1H, Hβ€”C(2)); 4.20–4.10 (m, 1H, Hβ€”C(4)); 3.80–3.65 (m, 4H, Hβ€”C(5), H3Cβ€”O); 3.53–3.41 (m, 1H, Hβ€”C(5)); 2.54–2.39 (m, 1H, Hβ€”C(3)); 2.21–2.12 (m, 1H, Hβ€”C(3)); 1.47+1.41 (2s, 9H, tBu). 13C-NMR (150 MHz, CDCl3): 172.2+171.9 (2s, COOMe); 153.9+153.4 (2s, COOtBu); 80.5 (s, C-tBu); 59.2+58.2 (2d, C(4)); 57.7+57.3 (2d, C(2)); 52.4+52.2 (2q, Me); 51.2+50.7 (2t, C(5)); 36.0+35.0 (2t, C(3)); 28.3+28.2 (2q, tBu). EI-MS (70ev): 270.1 ([M]+); 227.1 ([M-CO2+H]+); 169.1 ([M-BOC+H]+);.

v,vi: 21.1 g (78 mmol) of the above intermediate was dissolved in a (3:1)-mixture of dioxane/water (500 ml) and SnCl2 (59.2 g, 4 eq, 0.31 mol) was added at 0Β° and the solution stirred for 30 min. and gradually brought to room temperature and stirred for another 5 h. After adjusting the pH to 8 with solid NaHCO3, alkyl chloroformate (41.5 ml, 5 eq, 0.39 mol) was added and the solution stirred at room temperature overnight. The reaction mixture was evaporated and extracted with AcOEt. The organic phase was washed with brine, dried (Na2SO4), the solvent evaporated and the product was dried at high vacuum: (2S,4S)-4-[(Allyloxy)carbonylamino]-1-[(tert-butoxy)carbonyl]proline methylester (211) as a clear thick oil (22.3 g, 87%). [Ξ±]D20=βˆ’30.2Β° (c=1.25, CHCl3). 1H-NMR (300 MHz, CDCl3): 5.98–5.77 (m, 1H, Hβ€”C(Ξ²)(Alloc)); 5.32–5.12 (m, 2H, H2β€”C(Ξ³)(Alloc); 4.59–4.46 (m, 2H, H2β€”C(Ξ±)(Alloc)); 4.40–4.16 (m, 2H, Hβ€”C(4), Hβ€”C(2)); 3.80–3.53 (m, 4H, Hβ€”C(5), H3Cβ€”O); 3.53–3.31 (m, 1H, Hβ€”C(5)); 2.54–2.17 (m, 1H, Hβ€”C(3)); 1.98–1.84 (m, 1H, Hβ€”C(3)); 1.41+1.37 (2s, 9H, tBu). ESI-MS (MeOH+CH2Cl2): 351.2 ([M+Na]+); 229.0 ([M-BOC+H]+).

vii-ix: 22 g, 67 mmol) of 211 was dissolved in a (4:1)-mixture of methanol/water (100 ml) and LiOH (5 g, 2 eq, 134 mmol) was added at room temperature and the solution stirred for 3.5 h. The reaction mixture was evaporated and extracted with 1N hydrochloric acid (100 ml) and AcOEt. The solvent was removed and the resulting solid dissolved in 1:1 TFA/CH2Cl2 (200 ml) and stirred for 2 h. The solvents were evaporated and the product dried at high vacuum: (2S,4S)-4-[(Allyloxy)carbonylamino]proline as a clear oil (21 g, 96%) 1H-NMR (600 MHz, MeOH-d4): 5.98–5.85 (m, 1H, Hβ€”C(Ξ²)(Alloc)); 5.30 (dd, J=17.1, 1.5 Hz, 1H, Hβ€”C(Ξ³)(Alloc)); 5.12 (d, J=10.7 Hz, 1H, Hβ€”C(Ξ³)(Alloc)); 4.54 (d, J=4.4 Hz, 2H, H2β€”C(Ξ±)(Alloc)); 4.44 (t, J=8.9 Hz, 1H, Hβ€”C(2)); 4.36–4.27 (m, 1H, Hβ€”C(4)); 3.58 (dd, 3=12.2, 7.3 Hz, 1H, Hβ€”C(5)); 3.34–3.32 (m, 1H, Hβ€”C(5)); 2.73 (ddd, J=13.6, 8.7, 7.2 Hz, 1H, Hβ€”C(3)); 2.23–2.15 (m, 1H, Hβ€”C(3)). 13C-NMR (150 MHz, MeOH-d4): 171.3 (s, COOMe); 158.3 (s, COOAllyl); 134.1 (d, C(Ξ²)(Alloc)); 118.0 (t, C(Ξ³)(Alloc)); 66.8 (t, C(Ξ±)(Alloc)); 59.7 (d, C(2)); 51.3 (d, C(4)); 51.1 (t, C(5)); 34.9 (t, C(3)). ESI-MS (DCM+MeOH): 237.0 ([M+Na]+); 215.0 ([M+H]+).

15 g (70 mmol) of the above intermediate and 9-fluorenylmethoxycarbonylsuccinimid (28 g, 1.2 eq, 84 mmol) were dissolved in DCM (700 ml) and DIEA (48 ml, 6 eq, 0.42 mol) was added and the solution stirred overnight at room temperature. The solvent was removed and the residue dissolved in AcOEt and washed with 1N hydrochloric acid and dried (Na2SO4). After evaporation, the crude product was purified by filtration on silica gel with a gradient of (3:1) hexane/AcOEt to AcOEt. The solvent was evaporated and the residue crystallized from hexane at βˆ’20Β° C. The product was dried at high vacuum: (2S,4S)-4-[(Allyloxy)carbonylamino]-1-[(9H-fluoren-9-yl)methoxycarbonyl]-proline (212) as a white solid (23.8 mg, 78%) [Ξ±]D20=βˆ’27.0 (c=1.1, CHCl3). IR (KBr): 3321w (br.), 3066w, 2953w, 1707s, 1530m, 1451s, 1422s, 1354m, 1250m, 1205m, 1173m, 1118m, 1033m, 977m, 936m, 759m, 739s, 621m, 597w, 571w, 545s. 1H-NMR (300 MHz, MeOH-d4): 7.88–7.78 (m, 2H, Hβ€”C(4β€²)(Fmoc)); 7.71–7.61 (m, 2H, Hβ€”C(1β€²)(Fmoc)); 7.49–7.29 (m, 4H, Hβ€”C(3β€²)(Fmoc), Hβ€”C(2β€²)(Fmoc)); 6.08–5.68 (m, 1H, Hβ€”C(Ξ²)(Alloc)); 5.41–5.17 (m, 2H, H2β€”C(Ξ³)(Alloc); 4.58 (s, 2H, H2C(Ξ±)(Alloc)); 4.74–4.17 (m, 5H, H2-(10β€²)(Fmoc), Hβ€”C(9β€²)(Fmoc), Hβ€”C(4), Hβ€”C(2)); 3.94–3.73 (m, 1H, Hβ€”C(5)); 3.41–3.26 (m, 1H, Hβ€”C(5)); 2.74–2.54 (m, 1H, Hβ€”C(3)); 2.12–1.92 (m, 1H, Hβ€”C(3)). ESI-MS (DCM+MeOH): 459.3 ([M+Na]+); 437.3 ([M+H]+).


2.2. (2R,4S)-4-[(Allyloxy)carbonylamino]-1-[(9H-fluoren-9-yl)methoxycarbonyl]-proline (217)

i: A solution of acetic anhydride (1.02 kg, 5.3 eq, 10 mol) in glacial acetic acid (3 l) was heated to 50Β° C. and (2S,4R)-4-hydroxyproline (208) (247 g, 1.88 mol) was added in one portion. The solution was refluxed for 5.5 h, cooled to room temperature and the solvent was removed under reduced pressure giving a thick oil. The oil was then dissolved in 2N hydrochloric acid (3.5 l) and heated to reflux for 4 h and treated with charcoal and filtered through Celite. As the solution was evaporated, white needles formed, which were filtered. The product was dried at high vacuum: (2R,4R)-4-hydroxyproline.hydrochloride (213) white cryst. needles (220.9 g, 70%). M.p.: 117Β° C. [Ξ±]D20=+19.3Β° (c=1.04, water). IR (KBr): 3238s 3017s, 2569m, 1712s, 1584m, 1376s, 1332m, 1255s, 1204m, 1181w, 1091w, 1066w, 994w, 725m, 499s. 1H-NMR (600 MHz, MeOH-d4): 9.64 (s, 1H, Hβ€”N); 8.89 (s, 1H, Hβ€”N); 4.55–4.53 (m, 1H, Hβ€”C(4)); 4.51 (dd, J=10.4, 3.6 Hz, 1H, Hβ€”C(2)); 3.44–3.35 (m, 2H, H2β€”C(5)); 2.54–2.48 (m, 1H, Hβ€”C(3)); 2.40–2.34 (m, 1H, Hβ€”C(3)). 13C-NMR (150 MHz, MeOH-d4): 171.9 (s, COOH); 70.3 (d, C(4)); 59.6 (d, C(2)); 55.0 (t, C(5)); 38.5 (t, C(3)). EI-MS (NH3): 132.1 ([M-Cl]+). The filtrate was further concentrated to give an additional 59.5 g (19%).

ii,iii: To a solution of 213 (30 g, 0.18 mol) in abs. methanol (550 ml) was added dropwise at 0Β° C. thionyl chloride (38 ml, 2.5 eq, 0.45 mol). The solution refluxed for 3 h under nitrogen atmosphere. The solution was evaporated and the ester hydrochloride precipitated by adding diethylether. After filtration the white solid was washed with diethylether and dried at high vacuum: (2R,4R)-4-hydroxyproline methylester.hydrochloride white solid (29 g, 89%). [Ξ±]D20=+8.6Β° (c=0.873, MeOH). IR (KBr): 3388s (br.), 2980s (r.), 1730s, 1634m, 1586s, 1384s, 1248s, 1095s, 1064s, 1030m, 877m. 1H-NMR (300 MHz, MeOH d): 4.59–4.44 (m, 2H, Hβ€”C(4), Hβ€”C(2)); 3.81 (s, 3H, H3C-0); 3.37–3.31 (m, 2H, H2β€”C(5)); 2.50–2.37 (m, 1H, Hβ€”C(3)), 2.37–2.27 (m, 1H, Hβ€”C(3)). 13C-NMR (75 MHz, MeOH-d4): 170.9 (s, COOMe); 70.2 (d, C(4)); 59.8 (d, C(2)); 55.1 (t, C(5));)); 54.1 (q, C(Me)); 38.4 (1, C(3)). EI-MS (NH3): 146.1 ([M-Cl]+).

10 g (55 mmol) of the above intermediate was dissolved in CH2Cl2 (100 ml), cooled to 0Β° C. and triethylamine (15.2 ml, 2 eq, 0.11 mol) was added dropwise. Then di-tert.-butyldicarbonate (18.0 g, 1.5 eq, 83 mmol) in CH2Cl2 (10 ml) and 4-N,N-dimethylaminopyridine (0.67 g, 0.1 eq, 5 mmol) were added and the solution was stirred at RT overnight. The solution was washed with 1M aq. citric acid solution and sat. aqueous NaHCO3 solution, dried (Na2SO4), the solvents evaporated and dried at high vaccum: (2R,4R)-4-hydroxy-1-[(tert-butoxy)-carbonyl]prolinemethylester (214) as a white solid (13 g, 97%). [Ξ±]D20=+13.0Β° (c=1.06, CHCl3). IR (KBr): 3466s (br.), 2985s, 2930m, 1729s, 1679s, 1424s, 1283m, 1262m, 1122s, 1089s, 969m, 770m. 1H-NMR (300 MHz, CDCl3): 4.43–4.26 (m, 2H, Hβ€”C(4), Hβ€”C(2)); 3.80+3.79 (2s, 3H, H3Cβ€”O)); 3.76–3.47 (m, 2H, H2β€”C(5)); 2.44–2.24 (m, 1H, Hβ€”C(3)); 2.16–2.03 (m, 1H, Hβ€”C(3)); 1.47+1.43 (2s, 9H, tBu). ESI-MS: 268.1 ([M+Na]+).

iv,v: 214 (12.2 g, 50 mmol) was dissolved in CH2Cl2 (130 ml), cooled to 0Β° C. and 4-nitrobenzenesulfonyl chloride (14.3 g, 1.3 eq, 65 mmol) and Et3N (10.3 ml, 1.5 eq, 75 mmol) were added The reaction mixture was stirred overnight and gradually brought to room temperature. The solution was washed with 1N hydrochloric acid and saturated aqueous NaHCO3 solution, dried (Na2SO4), the solvents were evaporated and the crude product was purified by filtration on silica gel with (2:1)-mixture of hexane/AcOEt: 18 g (84%). The product was then recrystallized from hexane/AcOEt: (2R,4R)-4-[(p-nitrobenzyl)sulfonyloxy]-1-[(tert-butoxy)carbonyl]proline-methylester as white crystals (13.7 g, 64%). TLC (hexane/AcOEt 1:1): Rf 0.76. M.p.: 113–115Β° C. [Ξ±]D20=+21.6Β° (c=0.924, CHCl3). IR (KBr): 3112s (br.), 2981s, 2955s, 2882m, 1755s, 1683s, 1532s, 1413s, 1375s, 1348s, 1192s, 928s, 911s, 759m, 745s, 610s. 1H-NMR (600 MHz, CDCl3): 8.45–8.35 (m, 2H, Hβ€”C(Nos)); 8.15–8.06 (m, 2H, Hβ€”C(Nos)); 5.27–5.16 (m, 1H, Hβ€”C(4)); 4.53–4.32 (m, 1H, Hβ€”C(2)); 3.75–3.60 (m, 5H, H2β€”C(5), H3Cβ€”O); 2.59–2.35 (m, 2H, H2C(3)); 1.42+1.39 (2s, 9H, tBu). 13C-NMR (150 MHz, CDCl3): 171.8+171.6 (s, COOMe); 153.8+153.4 (s, COOtBu); 151.0+142.6 (s, C(Nos)); 129.2+124.7 (d, C(Nos)); 81.0 (s, C-tBu); 80.8+79.7 (d, C(4)); 57.4+57.1 (d, C(2)); 52.6+52.5+52.3+51.8 (t, C(5), q, Me); 37.2+36.3 (t, C(3)); 28.5+28.3 (q, tBu). ESI-MS (DCM+MEOH+NaI): 453.2 ([M+Na]+).

13 g (30 mmol) of the above intermediate was dissolved in DMF (200 ml), heated to 40Β° C. and sodium azide (14.3 g, 6 eq, 180 mmol) was added and the reaction mixture stirred over-night. The reaction mixture was evaporated and the residue suspended in diethylether. The suspension was filtered, the filtrate washed with water and the organic phase dried(Na2SO4). The solvent was evaporated and the product dried at high vacuum: (2R,4S)-4-azido-1-[(tert-butoxy)carbonyl]prolinemethylester (215) as a yellow oil (8.15 g, 99%). [Ξ±]D20=+42.8Β° (c=1.05, CHCl3). 1H-NMR (300 MHz, CDCl3): 4.58–4.37 (n, 1H, Hβ€”C(2)); 4.34–4.23 (m, 1H, Hβ€”C(4)); 3.92–3.51 (m, 5H, H2β€”C(5), H3Cβ€”O); 2.52–2.33 (m, 1H, Hβ€”C(3)); 2.33–2.20 (m, 1H, Hβ€”C(3)); 1.56+1.51 (2s, 9H, tBu). CI-MS (NH3): 288.2 ([M+NH4]+); 271.1 ([M+H]+).

vi,vii: 215 (8 g, 30 mmol) was dissolved in a (3:1)-mixture of dioxane/water (400 ml), cooled to 0Β° C. and SnCl2 (22.4 g, 4 eq, 120 mmol) was added and the reaction mixture stirred for 30 min. at 0Β°, gradually warmed to room temperature and stirred for another 5 h. After adjusting the pH of the solution to 8 with solid NaHCO3, alkyl chloroformate (15.7 ml, 5 eq, 150 mmol) was added. The reaction mixture was stirred overnight at room temperature, evaporated and extracted with AcOEt and the organic phase washed with brine. After drying the organic phase (Na2SO4), the solvent was evaporated and the product dried at high vacuum: (2R,4S)-4-[(Allyloxy)carbonylamino]-1-[(tert-butoxy)carbonyl]proline-methylester as a clear thick oil (216) (8.7 g, 89%). [Ξ±]D20=+41.9Β° (c=0.928, CHCl3). 1H-NMR (300 MHz CDCl3): 5.98–5.87 (m, 1H, Hβ€”C(Ξ²)(Alloc)); 5.34–5.02 (m, 2H, H2β€”C(Ξ³)(Alloc); 4.62–4.49 (m, 2H, H2β€”C(Ξ±)(Alloc)); 4.4–14.23 (m, 2H, Hβ€”C(4), Hβ€”C(2)); 3.82–3.66 (m, 4H, Hβ€”C(5), H3Cβ€”O); 3.43–3.20 (m, 1H, Hβ€”C(5)); 2.33–2.07 (m, 2H, H2β€”C(3)); 1.43+1.39 (2s, 9H, tBu). CI-MS (NH3): 329.1 ([M+H]+).

vii-x: 216 (8.4 g, 25 mmol) was dissolved in (4:1)-mixture of methanol/water (100 ml) at room temperature, LiOH (2.2 g, 2 eq, 50 mmol) added and the solution stirred overnight. Methanol was evaporated and the residue poured onto 1N hydrochloric acid (100 ml) and extracted with AcOEt. The solvent was removed and the residue dissolved in (1:1)-mixture of TFA/CH2Cl2 (200 ml) and stirred for 2 h. The solvents were evaporated and the product dried at high vaccum: (2R,4R)-4-[(Allyloxy)carbonylamino]proline as a clear oil (5.2 g, 96%) 1H-NMR (300 MHz MeOH-d4): 6.04–5.88 (m, 1H, H2β€”C(Ξ²)(Alloc)); 5.38–5.19 (m, 2H, H2β€”C(Ξ³)(Alloc); 4.64–4.54 (m, 3H, H2C(Ξ±)(Alloc), Hβ€”C(4)); 4.39–4.22 (m, 1H, Hβ€”C(2)); 3.71–3.60 (m, 1H, Hβ€”C(5)); 3.45–3.32 (m, 1H, Hβ€”C(5)); 2.51–2.41 (m, 2H, H2C(3)). CI-MS (NH3): 215.1 ([M+H]+).

200 mg (0.86 mmol) of the above intermediate and 9-fluorenylmethoxycarbonylsuccinimide (440 mg, 1.5 eq, 1.3 mmol) were dissolved in CH2Cl2 (10 ml) and DIEA (466 ΞΌl, 4 eq, 3.44 mmol) was added, and the solution stirred overnight at room temperature. The solvent was removed and the residue dissolved in AcOEt, washed with 1N hydrochloric acid dried (Na2SO4). After evaporation, the crude product was purified by filtration over silica gel with first a gradient of (3:1) hexane/AcOEt to AcOEt. The solvent was coevaporated with CH2Cl2 and the product dried at high vacuum: (2R,4S)-4-[(Allyloxy)carbonylamino]-1-[(9H-fluoren-9-yl)methoxycarbonyl]-proline (217) white solid (90 mg, 33%) [Ξ±]D20=+29.3Β° (c=1.08, CHCl3). IR (KBr): 3314s (br.), 3066s (br.), 2952s (br.), 1708s (br.), 1536m, 1424s, 1353s, 1126m, 1030 m, 909m, 759m, 738s, 620m. 1H-NMR (300 MHz, CDCl3): 8.74 (s, 1H, Hβ€”N); 7.79–7.66 (m, 2H, Hβ€”C(4β€²)(fmoc)); 7.62–7.49 (m, 2H, Hβ€”C(1β€²)(fmoc)); 7.44–7.22 (m, 4H, Hβ€”C(3β€²)(fmoc), Hβ€”C(2β€²)(fmoc)); 6.03–5.74 (m, 1H, Hβ€”C(Ξ²)(Alloc)); 5.41–5.07 (m, 2H, H2β€”C(Ξ³)(Alloc); 4.74–4.17 (m, 7H, H2β€”C(10β€²)(fmoc), Hβ€”C(9β€²)(fmoc), Hβ€”C(4), Hβ€”C(2), H2β€”C(Ξ±)(Alloc)); 3.91–3.76 (m, 1H, Hβ€”C(5)); 3.48–3.25 (m, 1H, Hβ€”C(5)); 2.45–2.08 (m, 2H, H2β€”C(3)). ESI-MS (MeOH): 437.3 ([M+H]+); ESI-MS (MeOH+Na): 459.1 ([M+Na]+).

2.3. Starting from derivatives 210 and 215 the key precursors 219a–u and 221a–u can be prepared according to Scheme 44.

R64: n-hexyl (219a, 221a); n-heptyl (219b, 221b); 4-(phenyl)benzyl (219c, 221c); diphenylmethyl (219d, 221d); 3-amino-propyl (219e, 221e); 5-amino-pentyl (219f, 221f); methyl (219 g, 221g); ethyl (219h, 221h); isopropyl (219I, 221i); isobutyl (219k, 221k); n-propyl (219l, 221l); cyclohexyl (219m, 221m); cyclohexylmethyl (219n, 221n); n-butyl (219o, 221o); phenyl (219p, 221p); benzyl (219q, 221q); (3-indolyl)methyl (219r, 221r); 2-(3-indolyl)ethyl (219s, 221s); (4phenyl)phenyl (219t, 221t); n-nonyl (219u, 221u).


i,ii: Typical Procedures:

To a solution of 78 mmol of azides 210 and 215 in a (3:1)-mixture of dioxane/water (500 ml) was added at 0Β° C. SnCl2 (59.2 g, 4 eq, 0.31 mol) and the solution was stirred for 30 minutes. The reaction mixture was gradually warmed up to room temperature and stirred for another 5 hours. After adjusting the pH to 8 with solid NaHCO3, the reaction mixture was extracted with CH2Cl2, the organic fraction dried (MgSO4), evaporated and the residue dried under reduced pressure. The residue was dissolved in CH2Cl2 (300 ml), cooled to 4Β° with an ice bath, followed by addition of DIEA (20.0 ml, 117 mmol) and a solution of the appropriate acid chloride R64β€²COCl (101.0 mmol) in CH2Cl2 (50 ml) at 4Β° C. The reaction mixture was stirred for 1 hour at 4Β° and for 18 hours at room temperature and extracted with HCl aq. (0.5N, 200 ml) and CH2Cl2. The organic fraction was dried (MgSO4), evaporated and the residue chromatographed on SiO2 with gradients of ethylacetate/hexane yielding 218a–u and 220a–u, which were converted into the final products 219a–u and 221a–u as described for the conversion of 216 into 217. The overall yields were 50–60%.

Templates (b1):

Synthesis of (2S,6S,8aR)-8a-{[(tert.-butyl)oxycarbonyl]methyl}perhydro-5,8-dioxo-{[(9H-fluoren-9-yl)methoxycarbonyl]amino}-pyrrolo[1,2-a]pyrazine-6-acetic acid (222):

To a stirred solution of 250 mg (0.414 mmol) of alkyl {(2S,6S,8aR)-8a-[(tert.-butyl)oxycarbonyl]methyl}perhydro-5,8-dioxo-{[(9H-fluoren-9-yl)methoxycarbonyl]amino}-pyrrolo[1,2-a]pyrazin-6-acetate in a degassed mixture of dichloromethane/methanol (9:1, 3 ml) were added under argon 25 mg (0.0216 mmol) of tetrakis(triphenylphosphine)palladium, 0.05 ml of acetic acid and 0.025 ml of N-methylmorpholine. The reaction mixture was stirred for 48 hours at room temperature and poured onto water and dichloromethane. The organic phase was dried (MgSO4), evaporated and the residue chromatographed on SiO2 with dichloromethane/methanol (9:1) to yield 180 mg (77%) of (25,6S,8aR)-8a-{[(tert.-butyl)oxycarbonyl]methyl}perhydro-5,8-dioxo-{[(9H-fluoren-9-yl)-methoxycarbonyl]amino}-pyrrolo[1,2-a]pyrazine-6-acetic acid (222) as a white powder.

1H-NMR(300 MHz, DMSO-d6): 8.30 (s, 1H); 7.88 (d, J=7.2, 2H); 7.67 (d, J=7.4, 2H); 7.62 (br.s, 1H); 7.41 (t, J=7.2, 2H); 7.33 (t, J=7.4, 2H); 4.35–4.2 (m, 5H); 3.55 (br.d, J=6.3, 2H); 2.8–2.55 (m, 3H); 2.45–2.25 (m, 2H); 2.1–1.95 (m, 1H); 1.35 (s, 9H); MS(ESI): 586.1 (M+Na)+, 564.1 (M+H)+.

Experimental procedure described in W. Bannwarth, A. Knierzinger, K. MΓΌller, D. Obrecht, A. Trzeciak EP 0 592 791 A2, 1993.

3. Biological Methods

3.1. Preparation of the Peptides

Lyophilized peptides were weighed on a Microbalance (Mettler MT5) and dissolved in sterile water containing 0.01% acetic acid Tachyplesin was purchased from Bachem Ltd. (Bubendorf Switzerland).

3.2. Antimicrobial Activity of the Peptides

The antimicrobial activities of the peptides were determined by the standard NCCLS broth microdilution method (see ref 1, below) examined in sterile 96-wells plates (Nunclon polystyrene microtiter plates) in a total volume of 100 ΞΌl. Innocula of the microorganisms were prepared with 0.5 Mcfarland standard and then diluted into Mueller-Hinton (MH) broth to give appr. 106 colony forming units (CFU)/ml for bacteria or 5Γ—103 CFU/ml for Candida. Aliquots (50 ΞΌl) of the innocula were added to 50 ΞΌl of MH broth containing the peptide in serial twofold dilutions. The microorganisms used were Escherichia coli (ATCC 25922), Pseudomnonas aeruginosa (P. aeruginosa) (ATCC 27853), Stahylococcus aureus (ATCC 29213 and ATCC 25923) and Candida albicans. A selected number of peptides were screened for activity against a larger panel of gram-negative strains. These strains were; Escherichia coli ATCC 43827 and clinical isolates of Pseudomonas (P. aeruginosa V07 14482, P. aeruginosa 15288, P. aeruginosa V02 15328 and P. aeruginosa V09 16085) and Acinetobacter (Acinetobacter V04 19905/1, Acinetobacter V12 21143/1 and Acinetobacter V12 21193/1). Antimicrobial activities of the peptides were expressed as the minimal inhibitory concentration (MIC) in jig/min at which no visible growth was observed after 18–20 hours of incubation of the microtiter plates at 37Β° C.

3.3. Antimicrobial Activity of the Peptides in 1% Salt

Salt sensitivity of the peptides was tested by the microtiter serial dilution assay as described above. Only MH broth was replaced by MH broth containing 1% NaCl.

3.4. Antimicrobial Activity of the Peptides in Human Serum

Serum binding of the peptides was tested by microtiter serial dilution assay as described above. Only MH broth was replaced by MH broth containing 90% human serum (BioWhittaker).

3.5. Hemolysis

The peptides were tested for their hemolytic activity against human red blood cells (hRBC). Fresh hRBC were washed three times with phosphate buffered saline (PBS) by centrifugation for 10 min at 2000Γ—g. Peptides at a concentration of 100 ΞΌg/ml were incubated with 20% v/v hRBC for 1 hour at 37Β° C. The final erythrocyte concentration was appr. 0.9Γ—109/ml. A value of 0% resp. 100% cell lysis was determined by incubation of the hRBC in the presence of PBS alone and resp. 0.1% Triton X-100 in H2O. The samples were centrifuged and the supernatant was 20 fold diluted in PBS buffer and the optical density (OD) of the sample at 540 nM was measured. The 100% lysis value (OD540H2O) gave an OD of approximately 1.6–2.0. Percent hemolysis was calculated as follows: (OD540peptide/OD540H2O)Γ—100%.

3.6. Cytotoxicity Assay

The cytotoxicity of the peptides to HELA cells (Acc57) and MCF-7 cells (Acc115) was determined using the MTT reduction assay (see ref 2 and 3, below). Briefly the method is as follows; HELA cells and MCF-7 cells were grown in RPMI1640 plus 5% fetal calf serum in microtiter plates for 48 hours at 37Β° C. at 5% CO2. The total number of cells was finally 106 cells per well. The supernatant of the cell cultures was discarded and fresh RPMI1640 medium containing 5% fetal calf serum and the peptides in serial dilutions of 12.5, 25 and 50 ΞΌg/ml were pipeted into the wells. Each peptide concentration was assayed in triplicate. Incubation of the cells was continued for 20–24 hours at 37Β° C. at 5% CO2. Wells were then washed three times with fresh RPMI medium and finally 100 ΞΌl MTT reagent (0.5 mg/ml in RPMI1640) was added to each well. This was incubated at 37Β° C. for 2 hours and subsequently the wells were washed once with PBS. 100 ΞΌl isopropanol was added to each well and the absorbance at 595 nm of the solubilized product was measured (OD595peptide). The 100 percent growth value (OD595Medium) was determined from wells containing HELA or MCF-7 cells with RPMI1640 plus 5% fetal calf serum but no peptides. The zero percent growth value (OD595Empty well) was extracted from wells that did not contain HELA or MCF-7 cells. The percentage MTT reduction for a certain peptide concentration was calculated as follows: (OD595peptide-OD595Empty well)/(OD595Medium-OD595Empty well)Γ—100% and was plotted for each peptide concentration. The EC50 of a peptide is defined as the concentration at which 50% inhibition of MTT reduction was observed and was calculated for each peptide.

REFERENCES

  • 1. National Committee for Clinical Laboratory Standards. 1993. Methods for dilution antimicrobial susceptibility tests for bacteria that grow aerobically, 3rd ed. Approved standard M7-A3. National Committee for Clinical laboratory standards, Villanova, Pa.
  • 2. Mossman T. J Immunol Meth 1983, 65, 55–63
  • 3. Berridge M V, Tan A S. Archives of Biochemistry & Biophysics 1993, 303, 474–482
    3.7. Results

TABLE 8
Minimal inhibitory concentrations (MIC in ΞΌg/ml) and percentage hemolyses at a
concentration of 100 ΞΌg/ml of peptide
Pseudomonas Staphylococcus Staphylococcus
Escherichia putida aureus aureus
coli ATCC ATCC ATCC ATCC Candida Hemolyses
Ex. 25922 27853 29213 25923 albicans hRBC
11 25 100 100 100 100 0.2
36 25 25 25 50 25 0.5
40 25 50 25 50 25 1.2
59 4.7 50 25 50 25 3.0
63 6.2 50 12.5 25 12.5 3.0
71 12.5 100 12.5 12.5 50 1.2
87 6.2 6.2 9.4 9.4 12.5 3.7
101 12.5 50 >50 >50 50 0.2
103 9.4 25 25 25 12.5 18.3
105 6.2 9.4 12.5 6.2 6.2 31.0
106 12.5 6.2 25 12.5 12.5 1.4
107 25 6.2 12.5 9.4 12.5 10.4
109 50 25 50 50 12.5 3.2
112 25 50 25 25 25 2.6
113 50 100 100 100 100 9.2
119 50 25 >100 100 50 3.5
120 18.8 9.4 18.8 9.4 12.5 1.1
121 25 25 6.2 6.2 6.2 7.1
126 25 25 25 50 25 2.6
128 6.2 12.5 6.2 6.2 12.5 13.9
133 6.2 6.2 12.5 25 12.5 1.1
134 12.5 6.2 12.5 25 12.5 1.2
137 25 6.2 6.2 6.2 6.2 3.1
139 25 6.2 12.5 9.4 6.2 3.5
140 12.5 6.2 12.5 12.5 6.2 2.7
141 25 12.5 25 25 12.5 2.0
142 25 12.5 50 25 12.5 2.3
146 12.5 12.5 25 12.5 6.2 30.1
147 50 25 25 25 12.5 1.9
148 25 12.5 12.5 9.4 6.2 3.9
150 25 12.5 12.5 12.5 12.5 29.3
151 50 50 100 50 25 4.9
152 25 25 50 25 12.5 29.1
154 12.5 12.5 25 12.5 12.5 31.5
155 6.2 12.5 6.2 12.5 6.2 10.1
156 50 12.5 12.5 6.2 12.5 35.2
158 12.5 6.2 12.5 12.5 12.5 10.5
159 12.5 12.5 12.5 12.5 12.5 21.7
161 25 12.5 6.2 6.2 12.5 3.7
163 12.5 12.5 12.5 12.5 12.5 24.6
165 6.2 12.5 25 18 12.5 0.2
168 12.5 12.5 25 25 12.5 1.1
172 6.2 25 25 25 12.5 1.0
173 12.5 25 6.2 12.5 12.5 27.4
175 12.5 6.2 12.5 12.5 12.5 2.4
177 25 12.5 25 25 12.5 4.1
182 12.5 6.2 6.2 25 12.5 6.2
185 12.5 6.2 6.2 6.2 12.5 17.6
186 6.2 3.1 6.2 6.2 6.2 11.5
187 12.5 100 50 100 25 0.3
197 12.5 3.1 6.2 6.2 6.2 3.4
203 6.2 6.2 6.2 6.2 6.2 33.0
205 6.2 6.2 12.5 6.2 6.2 27.0
206 6.2 6.2 12.5 12.5 6.2 8.5
207 50 50 25 50 25 0.1
208 12.5 6.2 6.2 6.2 12.5 18.4
209 12.5 6.2 12.5 12.5 18.8 6.4
210 12.5 6.2 25 25 25 1.9
214 12.5 6.2 12.5 12.5 12.5 1.0
216 12.5 6.2 12.5 25 12.5 1.4
217 18.8 6.2 12.5 25 12.5 1.7
218 25 6.2 25 25 25 2.2
219 12.5 12.5 50 50 25 2.6
220 12.5 18.8 25 25 12.5 2.3
222 12.5 6.2 12.5 12.5 6.2 2.2
223 6.2 12.5 12.5 25 12.5 2.7
224 6.2 12.5 18.8 25 12.5 3.7
225 6.2 12.5 12.5 25 12.5 4.4
228 12.5 6.2 6.2 6.2 12.5 6.3
229 12.5 6.2 3.1 6.2 6.2 4.8
230 6.2 6.2 6.2 9.4 12.5 1.7
232 6.2 12.5 9.4 6.2 9.4 1.5
233 9.4 12.5 9.4 6.2 12.5 37
234 6.2 12.5 6.2 3.1 12.5 33.9
242 6.2 12.5 6.2 12.5 12.5 19.4
244 3.1 12.5 6.2 6.2 12.5 22.7
250 6.2 6.2 12.5 12.5 12.5 0.7
251 6.2 9.4 6.2 12.5 12.5 4.1
254 12.5 6.2 6.2 12.5 12.5 11.7
256 3.1 3.1 6.2 6.2 6.2 2.7
257 6.2 6.2 6.2 6.2 25 19.6
258 6.2 6.2 6.2 6.2 12.5 23.6
259 6.2 6.2 6.2 6.2 12.5 18.0
267 12.5 6.2 6.2 12.5 12.5 3.4
277 25 18.8 3.1 6.2 6.2 12.7
278 12.5 25 50 50 50 5.3
279 12.5 12.5 50 50 50 4.9
280 12.5 12.5 50 100 25 1.8
281 12.5 4.7 100 100 50 1.1
282 12.5 12.5 25 50 25 1.6
283 12.5 4.7 100 100 50 1.0
284 6.2 1.6 12.5 12.5 12.5 0.7
287 25 50 12.5 25 25 28.5
288 25 1.5 100 100 100 1.1
289 50 3.1 25 25 25 1.7
292 25 6.2 50 100 25 1.3
293 25 12.5 100 100 100 1.3
294 25 3.1 100 100 50 1.5
295 25 6.5 50 100 50 2.0
296 12.5 6.2 25 50 25 1.9
297 25 3.1 100 100 50 0.9
298 25 3.1 100 200 50 1.0
299 50 6.2 25 100 50 2.5
300 25 12.5 12.5 25 50 6.5
301 25 50.0 50.0 25 50.0 0.5
302 6.2 3.1 3.1 6.2 6.2 3.4

TABLE 9
Minimal inhibitory concentration (MIC in ΞΌg/ml) in
Mueller-Hinton broth containing 1% NaCl
Escherichia Pseudomonas Staphylococcus Staphylococcus
coli putida aureus aureus
ATCC ATCC ATCC ATCC Candida
Ex. 25922 27853 29213 25923 albicans
106 100 50 100 100 100
197 12.5 6.2 18.8 12.5 12.5
230 25 50 50 50 18.8
250 12.5 50 100 50 50
229 50 18.8 25 25 12.5
256 6.2 6.2 25 25 25

Several compounds which showed a preference towards Gram-negative bacteria were tested against several pseudomonas strains as shown in Table 10.

TABLE 10
Minimal inhibitory concentrations (MIC in ΞΌg/ml) against pseudomonas strains
MIC (β–‘g/ml) ex. 197 ex. 284 ex. 283 ex. 288 ex. 289 ex. 292 ex. 296 ex. 297 ex. 298
Escherichia coli ATCC 25922 12.5 6.2 25 25 25 25 12.5 25 25
Escherichia coli ATCC 43827 12.5 12.5 12.5 12.5 25 25 12.5 12.5 12.5
P. aeruginosa ATCC 278853 3.1 1.6 3.1 3.1 6.2 6.2 3.1 3.1 3.1
P. aeruginosa VO7 14482 12.5 3.1 4.7 3.1 6.2 12.5 12.5 4.7 3.1
P. aeruginosa 15288 12.5 3.1 2.5 6.2 6.2 12.5 12.5 6.2 4.7
P. aeruginosa V02 15328 12.5 3.1 6.2 3.1 6.2 12.5 12.5 6.2 3.1
P. aeruginosa V09 16085 9.4 1.6 3.1 6.2 6.2 6.2 6.2 3.1 3.1
Acinetobacter V04 19905/1 12.5 6.2 6.2 6.2 12.5 12.5 6.2 6.2 6.2
Acinetobacter V12 21143/1 12.5 3.1 6.2 6.2 6.2 6.2 6.2 6.2 9.4
Acinetobacter V12 21193/1 12.5 3.1 3.1 6.2 3.1 6.2 3.1 6.2 6.2

TABLE 11
Anticancer activity (EC50-values) in ΞΌg/ml
Example Hemolysis
ex. Hela (ΞΌg/ml) MCF (ΞΌg/ml) hRBC
80 337 nd nd
106 43 39 1.4
170 24 41 nd
197 20 23 3.4
229 13 25 4.8
230 23 32 1.7
285 11 11 4.2
286 nd 23 17.1

Claims

The invention claimed is:

1. Compounds of the general formulae

wherein

is a group of the formulae

wherein

is the residue of an L-Ξ±-amino acid with B being the enantiomer of one of the groups A5, A8 or A10 as defined hereinafter;

is a group of one of the formulae

R1 is H; lower alkyl; or aryl-lower alkyl;

R2 is H; alkyl; alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sSR56; β€”(CH2)m(CHR61)sNR33R34; β€”(CH2)m(CHR61)sOCONR33R75; β€”(CH2)m(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;

R5 is alkyl; alkenyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)sNR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;

R7 is alkyl; alkenyl; β€”(CH2)q(CHR61)sOR55; β€”(CH2)q(CHR61)sNR33R34; β€”(CH2)q(CHR61)sOCONR33R75; β€”(CH2)q(CHR61)sNR20CONR33R82; β€”(CH2)r(CHR61)sCOOR57; β€”(CH2)r(CHR61)sCONR58R59; β€”(CH2)r(CHR61)sPO(OR60)2; β€”(CH2)r(CHR61)sSO2R62; or β€”(CH2)r(CHR61)sC6H4R8;

R8 is H; Cl; F; CF3; NO2; lower alkyl; lower alkenyl; aryl; aryl-lower alkyl; β€”(CH2)o(CHR61)sOR55; β€”(CH2)o(CHR61)sSR56; β€”(CH2)o(CHR61)NR33R34; β€”(CH2)o(CHR61)sOCONR33R75; β€”(CH2)o(CHR61)sNR20CONR33R82; β€”(CH2)o(CHR61)sCOOR57; β€”(CH2)o(CHR61)sCONR58R59; β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sCOR64;

R20 is H; alkyl; alkenyl; or aryl-lower alkyl;

R33 is H; alkyl, alkenyl; β€”(CH2)m(CHR61)sOR55; β€”(CH2)m(CHR61)sNR34R63; β€”(CH2)m(CHR61)sOCONR75R82; β€”CH2)m(CHR61)sNR20CONR78R82; β€”(CH2)o(CHR61)sCOR64; β€”(CH2)o(CHR61)sβ€”CONR58R59, β€”(CH2)o(CHR61)sPO(OR60)2; β€”(CH2)o(CHR61)sSO2R62; or β€”(CH2)o(CHR61)sC6H4R8;

R34 is H; lower alkyl; aryl, or aryl-lower alkyl;

R33 and R34 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;

R55 is H; lower alkyl; lower alkenyl; aryl-lower alkyl; β€”(CH2)m(CHR61)sOR57; β€”(CH2)m(CHR61)sNR34R63; β€”(CH2)m(CHR61)sOCONR75R82; β€”(CH2)m(CHR61)sNR20CONR78R82; β€”(CH2)o(CHR61)sβ€”COR64; β€”(CH2)o(CHR61)COOR57; or β€”(CH2)o(CHR61)sCONR58R59;

R56 is H; lower alkyl; lower alkenyl; aryl-lower alkyl; β€”(CH2)m(CHR61)sOR57; β€”(CH2)m(CHR61)sNR34R63; β€”(CH2)m(CHR61)sOCONR75R82; β€”(CH2)m(CHR61)sNR20CONR78R82; β€”(CH2)o(CHR61)sβ€”COR64; or β€”(CH2)o(CHR61)sCONR58R59;

R57 is H; lower alkyl; lower alkenyl; aryl lower alkyl; or heteroaryl lower alkyl;

R58 is H; lower alkyl; lower alkenyl; aryl; heteroaryl; aryl-lower alkyl; or heteroaryl-lower alkyl;

R59 is H; lower alkyl; lower alkenyl; aryl; heteroaryl; aryl-lower alkyl; or heteroaryl-lower alkyl; or

R58 and R59 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;

R60 is H; lower alkyl; lower alkenyl; aryl; or aryl-lower alkyl;

R61 is alkyl; alkenyl; aryl; heteroaryl; aryl-lower alkyl; heteroaryl-lower alkyl; β€”(CH2)mOR55; β€”(CH2)mNR33R34; β€”(CH2)mOCONR75R82; β€”(CH2)mNR20CONR78R82; β€”(CH2)oCOOR57; β€”(CH2)oNR58R59; or β€”(CH2)oPO(COR60)2;

R62 is lower alkyl; lower alkenyl; aryl, heteroaryl; or aryl-lower alkyl;

R63 is H; lower alkyl; lower alkenyl; aryl, heteroaryl; aryl-lower alkyl; heteroaryl-lower alkyl; β€”COR64; β€”COOR57; β€”CONR58R59; β€”SO2R62; or β€”PO(OR60)2;

R34 and R63 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;

R64 is H; lower alkyl; lower alkenyl; aryl; heteroaryl; aryl-lower alkyl; heteroaryl-lower alkyl; β€”(CH2)p(CHR61)sOR65; β€”(CH2)p(CHR61)sSR66; or β€”(CH2)p(CHR61)sNR34R63; β€”(CH2)P(CHR61)sOCONR75R82; β€”(CH2)p(CHR61)sNR20CONR78R82;

m is 2–4; o is 0–4; p is 1–4; q is 0–2; r is 1 or 2; s is 0 or 1;

R67 is H; Cl; Br; F; NO2; β€”NR34COR57; lower alkyl; or lower alkenyl;

R68 is H; Cl; Br; F; NO2; β€”NR34COR57; lower; or lower alkenyl;

R69 is H; Cl; Br; F; NO2; β€”NR34COR57; lower alkyl; or lower alkenyl; and

R70 is H; Cl; Br; F; NO2; β€”NR34COR57; lower alkyl; lower alkenyl;

Z is a chains of 12 Ξ±-amino acid residues, the positions of said amino acid residues in said chains being counted starting from the N-terminal amino acid, whereby these amino acid residues are, depending on their position in the chains, Gly, or of one of the types

C: β€”NR20CH(R72)COβ€”;

D: β€”NR20CH(R73)COβ€”;

E: β€”NR20CH(R74)COβ€”;

F: β€”NR20CH(R84)COβ€”; and

R72 is H; lower alkyl; lower alkenyl; β€”(CH2)p(CHR61)sOR85; or β€”(CH2)p(CHR61)sSR85;

R73 is β€”(CH2)oR77; β€”(CH2)rO(CH2)oR77; β€”(CH2)rS(CH2)oR77; or β€”(CH2)rNR20(CH2)oR77;

R74 is β€”(CH2)pNR78R79; β€”(CH2)pNR77R80; β€”(CH2)pC(═NR80)NR78R79; β€”(CH2)pC(═NOR50)NR78R79; β€”(CH2)pC(═NNR78R79)NR78R79; β€”(CH2)pNR80C(═NR80)NR78R79; β€”(CH2)pN═C(NR78R80)NR79R80; β€”(CH2)pC6H4NR78R79; β€”(CH2)pC6H4NR77R80; β€”(CH2)pC6H4C(═NR80)NR78R79; β€”(CH2)pC6H4C(═NORl)NR78R79; β€”(CH2)pC6H4C(═NNR78R79)NR78R79; β€”(CH2)pC6H4NR80C(═NR80)NR78R79; β€”(CH2)pC6H4N═C(NR78R80)NR79R80; β€”(CH2)rO(CH2)mNR78R79; β€”(CH2)rO(CH2)mNR77R80; β€”(CH2)rO(CH2)pC(═NR80)NR78R79; β€”(CH2)rO(CH2)pC(═NORl)NR78R79; β€”(CH2)rO(CH2)pC(═NNR78R79)NR78R79; β€”(CH2)rO(CH2)mNR80C(═NR80)NR78R79; β€”(CH2)rO(CH2)mN═C(NR78R80)NR79R80; β€”(CH2)rO(CH2)pC6H4CNR78R79; β€”(CH2)rO(CH2)pC6H4C(═NR80)NR78R79; β€”(CH2)rO(CH2)pC6H4C(═NORl)NR78R79; β€”(CH2)rO(CH2)pC6H4C(═NNR78R79)NR78R79; β€”(CH2)rO(CH2)pC6H4NR80C(═NR80)NR78R79; β€”(CH2)rS(CH2)mNR78R79; β€”(CH2)rS(CH2)mNR77R80; β€”(CH2)rS(CH2)pC(═NR80)NR78R79; β€”(CH2)rS(CH2)pC(═NORl)NR78R79; β€”(CH2)rS(CH2)pC(═NNR78R79)NR78R79; β€”(CH2)rS(CH2)mNR80C(═NR80)NR78R79; β€”(CH2)rS(CH2)mN═C(NR78R80)NR79R80; β€”(CH2)rS(CH2)pC6H4CNR78R79; β€”(CH2)rS(CH2)pC6H4C(═NR80)NR78R79; β€”(CH2)rS(CH2)pC6H4C(═NORl)NR78R79; β€”(CH2)rS(CH2)pC6H4C(═NNR78R79)NR78R79; β€”(CH2)rS(CH2)pC6H4NR80C(═NR80)NR78R79; β€”(CH2)pNR80COR64; β€”(CH2)pNR80COR77; β€”(CH2)pNR80CONR78R79; or β€”(CH2)pC6H4NR80CONR78R79;

R75 is lower alkyl; lower alkenyl; or aryl-lower alkyl;

R33 and R75 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;

R75 and R82 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;

R76 is H; lower alkyl; lower alkenyl; aryl-lower alkyl; β€”(CH2)oOR72; β€”(CH2)oSR72; β€”(CH2)oNR33R34; β€”(CH2)oOCONR33R75; β€”(CH2)oNR20CONR33R82; β€”(CH2)oCOOR75; β€”(CH2)oCONR58R59; β€”(CH2)oPO(OR60)2; β€”(CH2)pSO2R62; or β€”(CH2)oCOR64;

R77 is β€”C6R67R68R69R70R76; or a heteroaryl group of one of the formulae

R78 is H; lower alkyl; aryl; or aryl-lower alkyl;

R78 and R82 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;

R79 is H; lower alkyl; aryl; or aryl-lower alkyl; or

R78 and R79, taken together, can be β€”(CH2)2-7β€”; β€”(CH2)2O(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;

R80 is H; or lower alkyl;

R81 is H; lower alkyl; or aryl-lower alkyl;

R82 is H; lower alkyl; aryl; heteroaryl; or aryl-lower alkyl;

R33 and R82 taken together can form: β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”;

R83 is H; lower alkyl; aryl; or β€”NR78R79;

R84 is β€”(CH2)m(CHR61)sOH; β€”(CH2)pCONR78R79; β€”(CH2)pNR80CONR78R79; β€”(CH2)pC6H4CONR78R79; or β€”(CH2)pC6H4NR80CONR78R79;

R85 is lower alkyl; or lower alkenyl;

with the proviso that in said chain of 12 Ξ±-amino acid residues Z, the amino acid residues in positions 1 to 12 are:

P1: of type C or of type D or of type E or of type F;

P2: of type E or of type D;

P3: of type C or of type D;

P4: of type E or of type F or of type D;

P5: of type E or of type D or of type C, or the residue is Gly;

P6: of type E or of type F, or the residue is Gly;

P7: of type E or of type F;

P8: of type D or of type C;

P9: of type E or of type D or of type F;

P10: of type D or of type C;

P11: of type E or of type D; and

P12: of type C or of type D or of type E or of type F; and at P6 and P7 also D-isomers being possible;

and pharmaceutically acceptable salts thereof.

2. Compounds according to claim 1 wherein

R2 and R76 are other than β€”(CH2)m(CHR61)sOCONR33R75 or β€”(CH2)m(CHR61)sNR20CONR33R82;

R33, R55, R56, R61 and R64 are other than β€”(CH2)m(CHR61)sOCONR75R82 or β€”(CH2)m(CHR61)sNR20CONR78R82;

R33 and R34, or R34 and R63 are other than, taken together, β€”CH2-6β€”; β€”(CH2)2O(CH2)2β€”, β€”(CH2)2S(CH2)2β€” or β€”(CH2)2NR57(CH2)2β€”;

R57 in β€”(CH2)2NR57(CH2)2β€” or β€”(CH2)rNR57(CH2)rβ€” is other than lower alkenyl or heteroaryl-lower alkyl;

R74 is other than β€”(CH2)pNR77R80, β€”(CH2)pC6H4NR77R80, β€”(CH2)pO(CH2)mNR77R80, β€”(CH2)pS(CH2)mNR77R80, β€”(CH2)pN═C(NR78R80)NR79R80, β€”(CH2)pC6H4N═C(NR78R80)NR79R80, β€”(CH2)pO(CH2)mN═C(NR78R80)NR79R80, β€”(CH2)pS(CH2)mN═C(NR78R80)NR79R80, β€”(CH2)pNR80COR64, or β€”(CH2)pNR80COR77;

R77 is other than H52, H53 and H54; and

in Z the amino acid residues in positions 1, 5 and 12 are:

P1: of type C or of type D or of type E;

P5: of type E or of type D, or the residue is Gly; and

P12: of type C or of type D or of type E.

3. Compounds according to claim 1 wherein

R1 is hydrogen or lower alkyl;

R2 is H; lower alkyl; lower alkenyl; β€”(CH2)mOR55 (where R55 is lower alkyl; or lower alkenyl); β€”CH2)mSR56 (where R56 is lower alkyl; or lower alkenyl); β€”(CH2)mNR33R34 (where R33 is lower alkyl; or lower alkenyl; R34 is H; or lower alkyl; or R33 and R34 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)mOCONR33R75 (where R33 is H; lower alkyl; or lower alkenyl; R75 is lower alkyl; or R33 and R75 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)mNR20CONR33R82 (where R20 is H; or lower alkyl; R33 is H; or lower alkyl; or lower alkenyl; R82 is H; or lower alkyl; or R33 and R82 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20 is H; or lower alkyl; R64 is lower alkyl; or lower alkenyl); (CH2)oCOOR57 (where R57 is lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58 is lower alkyl; or lower alkenyl; and R59 is H; or lower alkyl; or R58 and R59 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60 is lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62 is lower alkyl; or lower alkenyl); or β€”(CH2)qC6F4R8 (where R8 is H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy);

R5 is lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55 is lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56 is lower alkyl; or lower alkenyl); (CH2)oNR33R34 (where R33 is lower alkyl; or lower alkenyl; R34 is H; or lower alkyl; or R33 and R34 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33 is H; or lower alkyl; or lower alkenyl; R75 is lower alkyl; or R33 and R75 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20 is H; or lower lower alkyl; R33 is H; or lower alkyl; or lower alkenyl; R82 is H; or lower alkyl; or R33 and R82 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where: R20 is H; or lower alkyl; R64 is alkyl; alkenyl; aryl; aryl-lower alkyl; or heteroaryl-lower alkyl); β€”(CH2)oCOOR57 (where R57 is lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58 is lower alkyl; or lower alkenyl; and R59 is H; or lower alkyl; or

R58 and R59 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60 is lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62 is lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8 is H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy):

R7 is lower alkyl; lower alkenyl; β€”(CH2)qOR55 (where R55 is lower alkyl; or lower alkenyl); β€”(CH2)qSR56 (where R56 is lower alkyl; or lower alkenyl); β€”(CH2)qNR33R34 (where R33 is lower alkyl; or lower alkenyl; R34 is H; or lower alkyl; or R33 and R34 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)qOCONR33R75 (where R33 is H; or lower alkyl; or lower alkenyl; R75 is lower alkyl; or R33 and R75 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)qNR20CONR33R82 (where R20 is H; or lower alkyl; R33 is H; or lower alkyl; or lower alkenyl; R82 is H; or lower alkyl; or R33 and R82 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)qN(R20)COR64 (where: R20 is H; or lower alkyl; R64 is lower alkyl; or lower alkenyl); β€”(CH2)rCOOR57 (where R57 is lower alkyl; or lower alkenyl); β€”(CH2)qCONR58R59 (where R58 is lower alkyl; or lower alkenyl; and R59 is H; or lower alkyl; or R58 and R59 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)rPO(OR60)2 (where R60 is lower alkyl; or lower alkenyl); β€”(CH2)rSO2R62 (where R62 is lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8 is H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy); R8 is H; F; Cl; CF3; lower alkyl; lower alkenyl; β€”(CH2)oOR55 (where R55 is lower alkyl; or lower alkenyl); β€”(CH2)oSR56 (where R56 is lower alkyl; or lower alkenyl); β€”(CH2)o(NR33R34 (where R33 is lower alkyl; or lower alkenyl; R34 is H; or lower alkyl; or R33 and R34 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oOCONR33R75 (where R33 is H; or lower alkyl; or lower alkenyl; R75 is lower alkyl; or R33 and R75 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oNR20CONR33R82 (where R20 is H; or lower alkyl; R33 is H; or lower alkyl; or lower alkenyl; R82 is H; or lower alkyl; or R33 and R82 taken together are β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oN(R20)COR64 (where R20 is H; or lower alkyl; R64 is lower alkyl; or lower alkenyl); β€”(CH2)oCOOR57 (where R57 is lower alkyl; or lower alkenyl); β€”(CH2)oCONR58R59 (where R58 is lower alkyl; or lower alkenyl; and R59 is H; or lower alkyl; or R58 and R59 taken together are β€”β€”(CH2)2-6β€”; β€”(CH2)2O(CH2)2β€”; β€”(CH2)2S(CH2)2β€”; or β€”(CH2)2NR57(CH2)2β€”; where R57 is H; or lower alkyl); β€”(CH2)oPO(OR60)2 (where R60 is lower alkyl; or lower alkenyl); β€”(CH2)oSO2R62 (where R62 is lower alkyl; or lower alkenyl); or β€”(CH2)qC6H4R8 (where R8 is H; F; Cl; CF3; lower alkyl; lower alkenyl; or lower alkoxy).

4. Compounds according to claim 3 wherein A is a group of one of the formulae A5 (with R2 being H); and A8.

5. Compounds according to claim 4 wherein A is a group of formula

wherein R20 is H or lower alkyl; and R64 is alkyl; alkenyl; aryl; aryl-lower alkyl; or heteroaryl-lower alkyl.

6. Compounds according to claim 5 wherein R64 is n-hexyl; n-heptyl; 4-(phenyl)benzyl; diphenylmethyl, 3-amino-propyl; 5-amino-pentyl; methyl; ethyl; isopropyl; isobutyl; n-propyl; cyclohexyl; cyclohexylmethyl; n-butyl; phenyl; benzyl; (3-indolyl)methyl; 2-(3-indolyl)ethyl; (4-phenyl)phenyl; or n-nonyl.

7. Compounds according to claim 1 wherein B is

an enantiomer of one of the groups A5 (with R2 being H) and A8.

8. Compounds according to claim 7 wherein B is a group, having (L)-configuration, of formula

wherein R20 is H; or lower alkyl; and R64 is alkyl; alkenyl; aryl; aryl-lower alkyl; or heteroaryl-lower alkyl.

9. Compounds according to claim 8 wherein R64 is n-hexyl; n-heptyl; 4-(phenyl)benzyl; diphenylmethyl, 3-amino-propyl; 5-amino-pentyl; methyl; ethyl; isopropyl; isobutyl; n-propyl; cyclohexyl; cyclohexylmethyl; n-butyl; phenyl; benzyl; (3-indolyl)methyl; 2-(3-indolyl)ethyl; (4-phenyl)phenyl; or n-nonyl.

10. Compounds according to claim 1 wherein in the chain of Ξ±-amino acid residues Z, the amino acid residues in position 1–12 are:

P1: of type C or of type E; or of type D; or of type F;

P2: of type E; or of type D;

P3: of type C or of type D;

P4: of type E;

P5: of type E; or of type C;

P6: of type E or of type F,

P7: of type E;

P8: of type D;

P9: of type E or of type D;

P10: of type D;

P11: of type E; or of type D and

P12: of type C or of type E; or of type D; or of type F;

at P6 and P7 also D-isomers being possible.

11. Compounds according to claim 10 wherein the amino acid residues in position 1–12 are:

P1: Leu; Arg; Lys; Tyr; Trp; Val; Gln; or 4-AmPhe;

P2: Mg; Trp; or Gln;

P3: Leu,; Val; Ile; or Phe;

P4: Lys; Arg; Gln; or Orn;

P5: Lys; or Arg;

P6: Arg; Tyr (Bzl); or DTyr (Bzl)

P7: Arg;

P8: Trp; Bip; 1-Nal; Tyr (Bzl); or Val;

P9: Lys; Arg; Orn; Tyr; Trp; or Gln;

P10: Tyr; Thr (Bzl); or Tyr (Bzl);

P11: Arg; or Tyr; and

P12: Val; Arg; 1-Nal; or 4-AmPhe.

12. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Arg; and

P12: Val.

13. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Y(Bzl);

P9: Lys;

P10: Tyr;

P11: Arg; and

P12: Val.

14. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Arg; and

P12: 1-Nal.

15. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Bip;

P9: Lys;

P10: Tyr;

P11: Arg; and

P12: Val.

16. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Thr (Bzl);

P11: Arg; and

P12: Val.

17. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Arg;

P10: Tyr;

P11: Arg; and

P12: Val.

18. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Trp;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Bip;

P9: Lys;

P10: Tyr;

P11: Arg; and

P12: Val.

19. A compound according to claim 1 wherein the template is DPro-(2R,4S)-4-[n-hexylcarbonylamino]-Lpro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Arg; and

P12: Val.

20. A compound according to claim 1 wherein the template is DPro-(2R,4S)-4-[cyclohexylcarbonylamino]-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Arg; and

P12: Val.

21. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Arg;

P2: Trp;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Tyr; and

P12: Val.

22. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Trp;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Tyr; and

P12: Arg.

23. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Arg;

P2: Trp;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Tyr; and

P12, Arg.

24. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: DTyr (Bzl);

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11, Arg; and

P12: Val.

25. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Arg;

P2: Bip;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Tyr; and

P12: Arg.

26. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Lys;

P2: Trp;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Tyr; and

P12: Arg.

27. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Tyr;

P2: Trp;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Tyr; and

P12: Arg.

28. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Trp;

P2: Trp;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Tyr; and

P12: Arg.

29. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Val;

P2: Trp;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Tyr; and

P12: Arg.

30. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Gln;

P2: Trp;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Arg;

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Tyr; and

P12: Arg.

31. A compound according to claim 1 wherein the template is DPro-LPro; and the amino acid residues in position 1–12 are:

P1: Leu;

P2: Arg;

P3: Leu;

P4: Lys;

P5: Lys;

P6: Tyr (Bzl);

P7: Arg;

P8: Trp;

P9: Lys;

P10: Tyr;

P11: Arg; and

P12: Val.

32. A pharmaceutical composition comprising a compound according to claim 1 and a pharmaceutically inert carrier.

33. A composition according to claim 32 in a form suitable for oral, topical, transdermal, injection, buccal, transmucosal, pulmonary or inhalation administration.

34. A composition according to claim 32 in form of tablets, dragees, capsules, solutions, liquids, gels, plasters, creams, ointments, syrups, slurries, suspensions, sprays, nebulisers or suppositories.

35. A process for the manufacture of compounds according to claim 1 comprising the steps of:

(a) coupling an appropriately functionalized solid support with an appropriately N-protected derivative of that amino acid which in the desired end-product is in position or 6, 7 or 5 any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;

(b) removing the N-protecting group from the product thus obtained;

(c) coupling the product thus obtained with an appropriately N-protected derivative of that amino acid which in the desired end-product is one position nearer the N-terminal amino acid residue, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;

(d) removing the N-protecting group from the product thus obtained;

(e) repeating steps (c) and (d) until the N-terminal amino acid residue has been introduced;

(f) coupling the product thus obtained to a compound of the general formula

wherein

is as defined above and X is an N-protecting group or, alternatively,

(fa) coupling the product obtained in step (d) or (e) with an appropriately N-protected derivative of an amino acid of the general formula


HOOCβ€”Bβ€”H  III


or


HOOC-A-H  IV

wherein B and A are as defined above , any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;

(fb) removing the N-protecting group from the product thus obtained; and

(fc) coupling the product thus obtained with an appropriately N-protected derivative of an amino acid of the above general formula IV and, respectively, III, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;

(g) removing the N-protecting group from the product obtained in step (f) or (fc);

(h) coupling the product thus obtained to an appropriately N-protected derivative of that amino acid which in the desired end-product is in position 12, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;

(i) removing the N-protecting group from the product thus obtained;

(j) coupling the product thus obtained to an appropriately N-protected derivative of that amino acid which in the desired end-product is one position farther away from position 12, any functional group which may be present in said N-protected amino acid derivative being likewise appropriately protected;

(k) removing the N-protecting group from the product thus obtained;

(l) repeating steps (j) and (k) until all amino acid residues have been introduced;

(m) if desired, selectively deprotecting one or several protected functional group(s) present in the molecule and appropriately substituting the reactive group(s) thus liberated;

(o) detaching the product thus obtained from the solid support;

(p) cyclizing the product cleaved from the solid support;

(q) removing any protecting groups present on functional groups of any members of the chain of amino acid residues and, if desired, any protecting group(s) which may in addition be present in the molecule; and

(r) if desired, converting the product thus obtained into a pharmaceutically acceptable salt or converting a pharmaceutically acceptable, or unacceptable, salt thus obtained into the corresponding free compound of formula I or into a different, pharmaceutically acceptable, salt.

Resources

Images & Drawings included:

Fig. 02 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 02
Fig. 03 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 04 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 05 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 06 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 06
Fig. 07 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 08 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 09 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 10 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 10
Fig. 100 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 100
Fig. 11 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 12 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 12
Fig. 13 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 14 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 15 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 16 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 17 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 18 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 19 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 20 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 21 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 22 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 23 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 24 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 25 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 26 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 27 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 27
Fig. 28 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 28
Fig. 29 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 29
Fig. 30 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 30
Fig. 31 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 31
Fig. 32 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 32
Fig. 33 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 33
Fig. 34 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 34
Fig. 35 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 35
Fig. 36 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 36
Fig. 37 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 37
Fig. 38 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 38
Fig. 39 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 39
Fig. 40 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 40
Fig. 41 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 41
Fig. 42 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 42
Fig. 43 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 43
Fig. 44 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 44
Fig. 45 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 45
Fig. 46 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 46
Fig. 47 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 47
Fig. 48 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 48
Fig. 49 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 49
Fig. 50 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 50
Fig. 51 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 51
Fig. 52 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 52
Fig. 53 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 53
Fig. 54 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 54
Fig. 55 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 55
Fig. 56 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 56
Fig. 57 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 57
Fig. 58 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 58
Fig. 59 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 59
Fig. 60 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 60
Fig. 61 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 61
Fig. 62 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 62
Fig. 63 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 63
Fig. 64 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 64
Fig. 65 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 65
Fig. 66 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 66
Fig. 67 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 67
Fig. 68 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 68
Fig. 69 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 69
Fig. 70 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 70
Fig. 71 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 71
Fig. 72 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 72
Fig. 73 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 73
Fig. 74 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 74
Fig. 75 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 75
Fig. 76 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 76
Fig. 77 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 77
Fig. 78 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 78
Fig. 79 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 79
Fig. 80 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 80
Fig. 81 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 81
Fig. 82 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 82
Fig. 83 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 83
Fig. 84 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 84
Fig. 85 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 85
Fig. 86 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 86
Fig. 87 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 87
Fig. 88 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 88
Fig. 89 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 89
Fig. 90 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 90
Fig. 91 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 91
Fig. 92 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 92
Fig. 93 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 93
Fig. 94 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 94
Fig. 95 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 95
Fig. 96 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 96
Fig. 97 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 98 - Template-fixed peptidomimetics with antimicrobial activity
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Fig. 99 - Template-fixed peptidomimetics with antimicrobial activity
Fig. 99

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