Differential effects of physiological agonists on the proteome of platelet‐derived extracellular vesicles

Author:

Moon Mitchell J.12ORCID,Rai Alin1345ORCID,Sharma Prerna12ORCID,Fang Haoyun13ORCID,McFadyen James D.2467ORCID,Greening David W.1345ORCID,Peter Karlheinz12458

Affiliation:

1. Department of Cardiometabolic Health University of Melbourne Melbourne Victoria Australia

2. Atherothrombosis and Vascular Biology Baker Heart and Diabetes Institute Melbourne Victoria Australia

3. Molecular Proteomics Baker Heart and Diabetes Institute Melbourne Victoria Australia

4. Central Clinical School Monash University Melbourne Victoria Australia

5. Baker Department of Cardiovascular Research Translation and Implementation La Trobe University Melbourne Victoria Australia

6. Department of Haematology Alfred Hospital Melbourne Victoria Australia

7. Australian Centre for Blood Diseases Monash University Melbourne Victoria Australia

8. Department of Cardiology Alfred Hospital Melbourne Victoria Australia

Abstract

AbstractArterial thrombosis manifesting as heart attack and stroke is the leading cause of death worldwide. Platelets are central mediators of thrombosis that can be activated through multiple activation pathways. Platelet‐derived extracellular vesicles (pEVs), also known as platelet‐derived microparticles, are granular mixtures of membrane structures produced by platelets in response to various activating stimuli. Initial studies have attracted interest on how platelet agonists influence the composition of the pEV proteome. In the current study, we used physiological platelet agonists of varying potencies which reflect the microenvironments that platelets experience during thrombus formation: adenosine diphosphate, collagen, thrombin as well as a combination of thrombin/collagen to induce platelet activation and pEV generation. Proteomic profiling revealed that pEVs have an agonist‐dependent altered proteome in comparison to their cells of origin, activated platelets. Furthermore, we found that various protein classes including those related to coagulation and complement (prothrombin, antithrombin, and plasminogen) and platelet activation (fibrinogen) are attributed to platelet EVs following agonist stimulation. This agonist‐dependent altered proteome suggests that protein packaging is an active process that appears to occur without de novo protein synthesis. This study provides new information on the influence of physiological agonist stimuli on the biogenesis and proteome landscape of pEVs.

Funder

National Heart Foundation of Australia

Publisher

Wiley

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