Platelet Distribution Width Is Associated with P-Selectin Dependent Platelet Function: Results from the Moli-Family Cohort Study

Author:

Izzi BenedettaORCID,Gialluisi AlessandroORCID,Gianfagna FrancescoORCID,Orlandi Sabatino,De Curtis Amalia,Magnacca Sara,Costanzo SimonaORCID,Di Castelnuovo Augusto,Donati Maria Benedetta,de Gaetano GiovanniORCID,Hoylaerts Marc F.ORCID,Cerletti ChiaraORCID,Iacoviello LiciaORCID,

Abstract

Defined as an index of platelet size heterogeneity, the platelet distribution width (PDW) is still a poorly characterized marker of platelet function in (sub)clinical disease. We presently validated PDW as a marker of P-selectin dependent platelet activation in the Moli-family cohort. Platelet-bound P-selectin and platelet/leukocyte mixed aggregates were measured by flow cytometry in freshly collected venous blood, both before and after in vitro platelet activation, and coagulation time was assessed in unstimulated and LPS- or TNFα-stimulated whole blood. Closure Times (CT) were measured in a Platelet Function Analyzer (PFA)-100. Multivariable linear mixed effect regression models (with age, sex and platelet count as fixed and family structure as random effect) revealed PDW to be negatively associated with platelet P-selectin, platelet/leukocyte aggregates and von Willebrand factor (VWF), and positively with PFA-100 CT, and LPS- and TNF-α-stimulated coagulation times. With the exception of VWF, all relationships were sex-independent. In contrast, no association was found between mean platelet volume (MPV) and these variables. PDW seems a simple, useful marker of ex vivo and in vitro P-selectin dependent platelet activation. Investigations of larger cohorts will define the usefulness of PDW as a risk predictor of thrombo-inflammatory conditions where activated platelets play a contributing role.

Funder

Telethon Foundation

Italian Ministry of University and Research

Fondazione Umberto Veronesi

Publisher

MDPI AG

Subject

General Medicine

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