Rational design of antithrombotic peptides to target the von Willebrand Factor (vWf) - GPIb integrin interaction |
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| Authors: | Carlos del Carpio Munoz William Campbell Iren Constantinescu Maria I. C. Gyongyossy-Issa |
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| Affiliation: | (1) Department of Applied Chemistry, Tohoku University, Sendai, Japan;(2) Biomime Solutions Inc., 4600 Westwater Dr., Richmond, BC, Canada;(3) Canadian Blood Services at UBC Centre for Blood Research, LSC - room 4.467, 2350 Health Sciences Mall, Vancouver, BC, V6T 1Z3, Canada;(4) Department of Pathology and Laboratory Medicine, at UBC Centre for Blood Research, 2350 Life Sciences Mall, Vancouver, BC, Canada |
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| Abstract: | ![]()
Conventional antithrombotic drug discovery requires testing of large numbers of drug candidates. We used computer-aided macromolecular interaction assessment (MIAX) to select antithrombotic molecules that mimic and therefore block platelet GPIb’s binding to von Willebrand factor (vWf), an early step in thrombus formation. We screened a random array of 15-mer D-amino acid peptides for binding vWf. Structures of 4 candidate peptides were inferred by comparison to sequences in protein databases, conversion from the L to D conformations and molecular dynamics (MD) determinations of those most energetically stable. By MIAX, we deduced the amino acids and intermolecular hydrogen bonds contributing to the GPIb-vWf interaction interface. We docked the peptides onto vWf in silico to localize their binding sites and consequent potential for preventing GPIb-vWf binding. In vitro inhibition of ristocetin-initiated platelet agglutination confirmed peptide function and suitability for antithrombotic development, thereby validating this novel approach to drug discovery. |
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| Keywords: | Antithrombotic design Computer-aided drug design GPIb-vWf interaction Molecular soft docking Peptide array Peptidomimetic Rational drug design |
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