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
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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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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
Structure of astacin and implications for activation of astacins and zinc-ligation of collagenases.
TL;DR: The X-ray crystal structure of astacin is reported, which reveals a deep active-site cleft, with the zinc at its bottom ligated by three histidines, a water molecule and a more remote tyrosine, which may represent the elusive 'third' zinc ligand in these enzymes.
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The c-proteinase that processes procollagens to fibrillar collagens is identical to the protein previously identified as bone morphogenic protein-1
TL;DR: It is demonstrated that procollagen C-proteinase is identical to BMP-1, a member of the "astacin families" of zinc-requiring endopeptidases that play critical roles in embryonic hatching, dorsal/ventral patterning, and early developmental decisions.
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Failure of ventral body wall closure in mouse embryos lacking a procollagen C-proteinase encoded by Bmp1, a mammalian gene related to Drosophila tolloid
Noboru Suzuki,Patricia A. Labosky,Yasuhide Furuta,Linda Hargett,Ray Dunn,Agnes B. Fogo,Kazuhiko Takahara,Donna M. P. Peters,Daniel S. Greenspan,Brigid L.M. Hogan +9 more
TL;DR: Analysis of the amnion of homozygous mutant embryos reveals the absence of the fold that normally tightly encloses the physiological hernia of the gut, consistent with the incorporation of partially processed procollagen molecules.
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In vivo significance of kinetic constants of protein proteinase inhibitors
TL;DR: In vivo significance of the kinetic parameters which characterize the interaction between proteinases and protein proteinase inhibitors are described and a stability time for enzyme-inhibitor complexes is defined as a minimal time during which the complexes may be considered as stable.