Phosphinic peptides, the first potent inhibitors of astacin, behave as extremely slow-binding inhibitors.
Irene Yiallouros,Stamatia Vassiliou,Athanasios Yiotakis,Robert Zwilling,Walter Stöcker,Vincent Dive +5 more
TLDR
The phosphinic peptides may provide a rational basis for the design of drugs directed towards other members of the astacin family which, like bone morphogenetic protein 1 (BMP1), have become targets of pharmacological research.Abstract:
A series of phosphinic pseudo-peptides varying in length and composition have been designed as inhibitors of the crayfish zinc endopeptidase astacin, the prototype of the astacin family and of the metzincin superfamily of metalloproteinases. The most efficient phosphinic peptide, fluorenylmethyloxycarbonyl-Pro-Lys-PhePsi(PO2CH2)Ala-P ro-Leu-Val, binds to astacin with a Ki value of 42 nM, which is about three orders of magnitude below the corresponding values for previously used hydroxamic acid derivatives. However, the rate constants for association (kon = 96.8 M-1.s-1) and dissociation (koff = 4.1 x 10(-6) s-1) are evidence for the extremely slow binding behaviour of this compound. N-terminally or C-terminally truncated phosphinic analogues of this parent molecule are much less potent, indicating a critical role of the peptide size on the potency. In particular, omission of the N-terminal proline residue leads to a 40-fold increase in Ki which is mostly due to a 75-fold higher koff value. These findings are consistent with the previously solved crystal structure of astacin complexed with one of the phosphinic peptides, benzyloxycarbonyl-Pro-Lys-PhePsi(PO2CH2)Ala-Pro-O-methyl, Ki = 14 microM [Grams, Dive, Yiotakis, Yiallouros, Vassiliou, Zwilling, Bode and Stocker (1996) Nature Struct. Biol. 3, 671-675]. This structure also reveals that the phosphinic group binds to the active site as a transition-state analogue. The extremely slow binding behaviour of the phosphinic peptides is discussed in the light of the conformational changes involving a unique 'tyrosine switch' in the structure of astacin upon inhibitor binding. The phosphinic peptides may provide a rational basis for the design of drugs directed towards other members of the astacin family which, like bone morphogenetic protein 1 (BMP1; i.e. the procollagen C-proteinase), have become targets of pharmacological research.read more
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Rationally designed anti-HER2/neu peptide mimetic disables P185HER2/neu tyrosine kinases in vitro and in vivo.
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Meprins, membrane-bound and secreted astacin metalloproteinases.
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RXP 407, a phosphinic peptide, is a potent inhibitor of angiotensin I converting enzyme able to differentiate between its two active sites
Vincent Dive,Joël Cotton,Athanasios Yiotakis,Annie Michaud,Stamatia Vassiliou,Jiri Jiracek,Gilles Vazeux,Marie-Thérèse Chauvet,Philippe Cuniasse,Pierre Corvol +9 more
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Sortase A: An ideal target for anti-virulence drug development
TL;DR: This review is focused on the most promising sortase A inhibitor compounds that are currently in development as leads towards a new class of anti-infective drugs that are urgently needed to help combat the alarming increase in antimicrobial resistance.
Sortase A : an ideal target for anti-virulence drug development
TL;DR: The most promising sortase A inhibitor compounds that are currently in development as leads towards a new class of anti-infective drugs that are urgently needed to help combat the alarming increase in antimicrobial resistance are presented in this paper.
References
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Journal ArticleDOI
Implications of the three‐dimensional structure of astacin for the structure and function of the astacin family of zinc‐endopeptidases
TL;DR: The topology of residues forming the zinc-binding active site of astacin corresponds to almost identical arrangements in all other astacins, suggesting that these are likewise metalloproteinases.
Journal ArticleDOI
Structure of chymotrypsin-trifluoromethyl ketone inhibitor complexes: comparison of slowly and rapidly equilibrating inhibitors.
TL;DR: The crystallographic structures of the complexes of gamma-chymotrypsin with inhibitors 1 and 2 have been determined in order to establish whether structural or conformational differences can be found which account for different kinetic and thermodynamic properties of the two inhibitors.
Journal ArticleDOI
Development of the First Potent and Selective Inhibitor of the Zinc Endopeptidase Neurolysin Using a Systematic Approach Based on Combinatorial Chemistry of Phosphinic Peptides
TL;DR: The efficiency of this novel approach in rapid identification of the first potent inhibitor of the mammalian zinc endopeptidase neurolysin (24-16) is demonstrated, able to discriminate between this enzyme and the related zinc endopesetidase thimet oligopePTidase ( 24-15).
Journal ArticleDOI
The slow, tight binding of bestatin and amastatin to aminopeptidases.
S H Wilkes,J M Prescott +1 more
TL;DR: The slow, tight binding observed with five of the six aminopeptidase-inhibitor pairs investigated suggests the formation of a transition state analog complex between the enzyme and inhibitor, and physical evidence consistent with this possibility was provided by the observation that both bestatin and amastatin perturb the absorption spectrum of cobalt Aeromonas am inopeptids.
Journal ArticleDOI
Crystal structure of a complex between Serratia marcescens metallo-protease and an inhibitor from Erwinia chrysanthemi.
U. Baumann,Margit Bauer,Margit Bauer,Margit Bauer,Sylvie Létoffé,Sylvie Létoffé,Sylvie Létoffé,Philippe Delepelaire,Philippe Delepelaire,Philippe Delepelaire,Cécile Wandersman,Cécile Wandersman,Cécile Wandersman +12 more
TL;DR: In this article, the crystal structure of the complex between the 50 kDa metallo-endo-proteinase from Serratia marcescens (SMP), a member of the metzincin superfamily, and an inhibitor from Erwinia chrysanthemi (Inh) was solved by molecular replacement using the known structure of SMP, and refined at 2.30 A resolution to a crystallographic R -factor of 0.195.