Effects of Platelet Agonists and Priming on the Formation of Platelet Populations

Author:

Veninga Alicia1,Baaten Constance C. F. M. J.12,De Simone Ilaria13,Tullemans Bibian M. E.1,Kuijpers Marijke J. E.14ORCID,Heemskerk Johan W. M.1ORCID,van der Meijden Paola E. J.14

Affiliation:

1. Department of Biochemistry, Cardiovascular Research Institute Maastricht, Maastricht University, The Netherlands

2. Institute for Molecular Cardiovascular Research, University Hospital Aachen, RWTH Aachen University, Germany

3. Institute for Cardiovascular and Metabolic Research, University of Reading, Reading, United Kingdom

4. Thrombosis Expertise Center, Heart and Vascular Center, Maastricht University Medical Center, Maastricht, The Netherlands

Abstract

AbstractPlatelets from healthy donors display heterogeneity in responsiveness to agonists. The response thresholds of platelets are controlled by multiple bioactive molecules, acting as negatively or positively priming substances. Higher circulating levels of priming substances adenosine and succinate, as well as the occurrence of hypercoagulability, have been described for patients with ischaemic heart disease. Here, we present an improved methodology of flow cytometric analyses of platelet activation and the characterisation of platelet populations following activation and priming by automated clustering analysis.Platelets were treated with adenosine, succinate, or coagulated plasma before stimulation with CRP-XL, 2-MeSADP, or TRAP6 and labelled for activated integrin αIIbβ3 (PAC1), CD62P, TLT1, CD63, and GPIX. The Super-Enhanced Dmax subtraction algorithm and 2% marker (quadrant) setting were applied to identify populations, which were further defined by state-of-the-art clustering techniques (tSNE, FlowSOM).Following activation, five platelet populations were identified: resting, aggregating (PAC1 + ), secreting (α- and dense-granules; CD62P + , TLT1 + , CD63 + ), aggregating plus α-granule secreting (PAC1 + , CD62P + , TLT1 + ), and fully active platelet populations. The type of agonist determined the distribution of platelet populations. Adenosine in a dose-dependent way suppressed the fraction of fully activated platelets (TRAP6 > 2-MeSADP > CRP-XL), whereas succinate and coagulated plasma increased this fraction (CRP-XL > TRAP6 > 2-MeSADP). Interestingly, a subset of platelets showed a constant response (aggregating, secreting, or aggregating plus α-granule secreting), which was hardly affected by the stimulus strength or priming substances.

Funder

Landsteiner Foundation for Blood Transfusion Research

The Dutch Heart Foundation

START-Program of the Faculty of Medicine at the RWTH Aachen University

Marie Sklodowska-Curie grant

Publisher

Georg Thieme Verlag KG

Subject

Hematology

Reference44 articles.

1. Platelet populations and priming in hematological diseases;C CFMJ Baaten;Blood Rev,2017

2. Platelet biology and functions: new concepts and clinical perspectives;P EJ van der Meijden;Nat Rev Cardiol,2019

3. Targeting platelet receptor function in thrombus formation: the risk of bleeding;F Swieringa;Blood Rev,2014

4. Expressions of adenosine A2A receptors in coronary arteries and peripheral blood mononuclear cells are correlated in coronary artery disease patients;V Gariboldi;Int J Cardiol,2017

5. Rapid measurement of adenosine concentration in human blood using FixedPotential amperometry: comparison with mass spectrometry and high-performance liquid chromatography;M Marlinge;J Anal Bioanal Tech,2017

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