Platelet activation and coronavirus disease 2019 mortality: Insights from coagulopathy, antiplatelet therapy and inflammation.

Arch Cardiovasc Dis

Innovative Therapies in Haemostasis, Inserm, université Paris Cité, 75006 Paris, France; Department of Haematology and Biosurgical Research Laboratory (Carpentier Foundation), hôpital européen Georges-Pompidou, AP-HP, AP-HP.CUP, Inserm UMR-S1140, 20, rue Leblanc, 75015 Paris, France. Electronic address:

Published: April 2023

The study examines the role of platelet activation in influencing mortality rates in COVID-19 patients by analyzing two patient cohorts for blood biomarkers related to platelet activity.
In cohort A of 208 patients, higher levels of soluble platelet biomarkers were noted in critical patients, linking them to increased in-hospital mortality; however, this association was not significant when adjusting for coagulopathy indicators.
Results from cohort B, which included nearly 2900 patients, indicated that prior use of antiplatelet medications did not significantly affect mortality outcomes, suggesting that coagulopathy may be a more critical factor in the progression of COVID-19.

Background: Coronavirus disease 2019 (COVID-19) is associated with an inflammatory cytokine burst and a prothrombotic coagulopathy. Platelets may contribute to microthrombosis, and constitute a therapeutic target in COVID-19 therapy.

Aim: To assess if platelet activation influences mortality in COVID-19.

Methods: We explored two cohorts of patients with COVID-19. Cohort A included 208 ambulatory and hospitalized patients with varying clinical severities and non-COVID patients as controls, in whom plasma concentrations of the soluble platelet activation biomarkers CD40 ligand (sCD40L) and P-selectin (sP-sel) were quantified within the first 48hours following hospitalization. Cohort B was a multicentre cohort of 2878 patients initially admitted to a medical ward. In both cohorts, the primary outcome was in-hospital mortality.

Results: In cohort A, median circulating concentrations of sCD40L and sP-sel were only increased in the 89 critical patients compared with non-COVID controls: sP-sel 40,059 (interquartile range 26,876-54,678)pg/mL; sCD40L 1914 (interquartile range 1410-2367)pg/mL (P<0.001 for both). A strong association existed between sP-sel concentration and in-hospital mortality (Kaplan-Meier log-rank P=0.004). However, in a Cox model considering biomarkers of immunothrombosis, sP-sel was no longer associated with mortality, in contrast to coagulopathy evaluated with D-dimer concentration (hazard ratio 4.86, 95% confidence interval 1.64-12.50). Moreover, in cohort B, a Cox model adjusted for co-morbidities suggested that prehospitalization antiplatelet agents had no significant impact on in-hospital mortality (hazard ratio 1.05, 95% CI 0.80-1.37; P=0.73).

Conclusions: Although we observed an association between excessive biomarkers of platelet activation and in-hospital mortality, our findings rather suggest that coagulopathy is more central in driving disease progression, which may explain why prehospitalization antiplatelet drugs were not a protective factor against mortality in our multicentre cohort.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9925415	PMC
http://dx.doi.org/10.1016/j.acvd.2023.01.006	DOI Listing

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