Kelly L. Hayes scite author profile

Kelly L. Hayes

3Publications

18Citation Statements Received

48Citation Statements Given

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University of Vermont

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The Platelet High Affinity Binding Site for Thrombin Mimics Hirudin, Modulates Thrombin-induced Platelet Activation, and Is Distinct from the Glycoprotein Ib-IX-V Complex

Hayes

Tracy

1999

Journal of Biological Chemistry

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The platelet high affinity binding site for thrombin appears to be described by a classical receptor-ligand interaction that is distinct from the platelet thrombin receptor/substrate, PAR-1. However, the identification and function of the high affinity binding site with respect to its physiological importance have continued to elude investigators. Prior studies using two mutant thrombins suggested that thrombin interaction with the platelet high affinity binding site is mediated through an extensive portion of the thrombin molecule involving residues within the substrate binding pocket and PAR-1 and GP Ib by three-color immunofluorescence using confocal microscopy. These combined studies demonstrate that the high affinity binding site for thrombin is a unique platelet protein distinct from GP Ib which modulates the effective thrombin concentration localized at the human platelet surface.

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alpha-Thrombin-induced human platelet activation results solely from formation of a specific enzyme-substrate complex.

Hayes

Leong

Henriksen

et al. 1994

Journal of Biological Chemistry

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1098-84 Persistently increased platelet reactivity prestages subsequent cardiac events after an acute coronary event

Hayes¹,

Godaire²,

Sobel³

et al. 2004

Journal of the American College of Cardiology

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Kelly L. Hayes

The Platelet High Affinity Binding Site for Thrombin Mimics Hirudin, Modulates Thrombin-induced Platelet Activation, and Is Distinct from the Glycoprotein Ib-IX-V Complex

alpha-Thrombin-induced human platelet activation results solely from formation of a specific enzyme-substrate complex.

1098-84 Persistently increased platelet reactivity prestages subsequent cardiac events after an acute coronary event

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