Abstract
Structure-activity studies have been pursued on cyclo-S,S-[Ac-Cys-(Nα-Me)Arg-Gly-Asp-Pen]- NH2,2 (SKF 106760), a potent inhibitor of platelet aggregation, in an effort to improve potency and affinity for the GPIIb/IIIa receptor. Modifications on the N- and C-termini of 2 produced a series of peptides which indicate that the C-terminal carboxylate group may be a secondary receptor-binding element. Further modification by replacing the disulfide tether Nα-acetylcysteine/penicillamineamide with the novel, inexpensive, achiral, constrained, and more lipophilic tether 2-mercaptobenzoyl/2-mercaptoaniline (Mba/Man) afforded the semipeptide cyclo-S,S- [Mba- (Nα-Me) Arg-Gly-Asp-Man], 18 (SKF 107260), which exhibited significant enhancement in both affinity and potency. To further investigate the effect of the phenyl ring at the C-terminus, peptides bearing the novel (2R,3S)- and (2R,3R)-β-phenylcysteines were synthesized, which culminated in the cyclo-S,S-[Ac-Cys-(Nα-Me)Arg-Gly-Asp-(2R,3S)-β-phenylCys]-OH peptide, 22, which displayed substantial affinity and potency. We describe, herein, the development of both 18 and 22 and the additional structural modifications within the constrained cyclic disulfide ring to probe the stereochemical and steric requirements for receptor interaction. © 1994, American Chemical Society. All rights reserved.
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CITATION STYLE
Ali, F. E., Bennett, D. B., Calvo, R. R., Elliott, J. D., Hwang, S. M., Ku, T. W., … Samanen, J. M. (1994). Conformationally Constrained Peptides and Semipeptides Derived from RGD as Potent Inhibitors of the Platelet Fibrinogen Receptor and Platelet Aggregation. Journal of Medicinal Chemistry, 37(6), 769–780. https://doi.org/10.1021/jm00032a009
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