Fibrin-glycoprotein VI interaction increases platelet procoagulant activity and impacts clot structure

Julia S Gauer; Cédric Duval; Rui-Gang Xu; Fraser L Macrae; Helen R McPherson; Christian Tiede; Darren Tomlinson; Steve P Watson; Robert A S Ariëns

doi:10.1016/j.jtha.2022.09.004

Fibrin-glycoprotein VI interaction increases platelet procoagulant activity and impacts clot structure

J Thromb Haemost. 2023 Mar;21(3):667-681. doi: 10.1016/j.jtha.2022.09.004. Epub 2022 Dec 22.

Authors

Julia S Gauer¹, Cédric Duval¹, Rui-Gang Xu¹, Fraser L Macrae¹, Helen R McPherson¹, Christian Tiede², Darren Tomlinson², Steve P Watson³, Robert A S Ariëns⁴

Affiliations

¹ Discovery and Translational Science Department, Leeds Institute of Cardiovascular and Metabolic Medicine, University of Leeds, Leeds, United Kingdom.
² School of Molecular and Cellular Biology, Faculty of Biological Sciences, University of Leeds, Leeds, United Kingdom.
³ Institute of Cardiovascular Sciences, College of Medical and Dental Sciences, University of Birmingham, Birmingham, United Kingdom.
⁴ Discovery and Translational Science Department, Leeds Institute of Cardiovascular and Metabolic Medicine, University of Leeds, Leeds, United Kingdom. Electronic address: R.A.S.Ariens@leeds.ac.uk.

PMID: 36696196
DOI: 10.1016/j.jtha.2022.09.004

Abstract

Background: The glycoprotein VI (GPVI) signaling pathway was previously reported to direct procoagulant platelet activity through collagen binding. However, the impact of GPVI-fibrin interaction on procoagulant platelet development and how it modulates the clot structure are unknown.

Objectives: To determine the effect of GPVI-fibrin interaction on the platelet phenotype and its impact on the clot structure.

Methods: Procoagulant platelets in platelet-rich plasma clots were determined by scanning electron microscopy (wild-type and GPVI-deficient murine samples) and confocal microscopy. Procoagulant platelet number, clot density, clot porosity, and clot retraction were determined in platelet-rich plasma or whole blood clots of healthy volunteers in the presence of tyrosine kinase inhibitors (PRT-060318, ibrutinib, and dasatinib) and eptifibatide.

Results: GPVI-deficient clots showed a higher nonprocoagulant vs procoagulant platelet ratio than wild-type clots. The fiber density and the procoagulant platelet number decreased in the presence of Affimer proteins, inhibiting GPVI-fibrin(ogen) interaction and the tyrosine kinase inhibitors. The effect of GPVI signaling inhibitors on the procoagulant platelet number was exacerbated by eptifibatide. The tyrosine kinase inhibitors led to an increase in clot porosity; however, no differences were observed in the final clot weight, following clot retraction with the tyrosine kinase inhibitors, except for ibrutinib. In the presence of eptifibatide, clot retraction was impaired.

Conclusion: Our findings showed that GPVI-fibrin interaction significantly contributes to the development of procoagulant platelets and that inhibition of GPVI signaling increases clot porosity. Clot contractibility was impaired by the integrin αIIbβ3 and Btk pathway inhibition. Thus, inhibition of GPVI-fibrin interactions can alleviate structural characteristics that contribute to a prothrombotic clot phenotype, having potential important implications for novel antithrombotic interventions.

Keywords: GPVI; clot structure; fibrin; procoagulant platelets; tyrosine kinase inhibitors.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Blood Platelets / metabolism
Eptifibatide / pharmacology
Fibrin* / chemistry
Mice
Platelet Membrane Glycoproteins / metabolism
Thrombosis*

Substances

Eptifibatide
Fibrin
Platelet Membrane Glycoproteins
platelet membrane glycoprotein VI

Abstract

Publication types

MeSH terms

Substances

Grants and funding