The Platelet Lipidome Is Altered in Patients with COVID-19 and Correlates with Platelet Reactivity

COVID-19 患者的血小板脂质组发生改变,且与血小板反应性相关

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作者:Alex R Schuurman, Valentine Léopold, Liza Pereverzeva, Osoul Chouchane, Tom D Y Reijnders, Justin de Brabander, Renée A Douma, Michel van Weeghel, Eric Wever, Bauke V Schomaker, Frédéric M Vaz, Willem Joost Wiersinga, Cornelis Van't Veer, Tom van der Poll

Background

Activated platelets have been implicated in the proinflammatory and prothrombotic phenotype of coronavirus disease 2019 (COVID-19). While it is increasingly recognized that lipids have important structural and signaling roles in platelets, the lipidomic landscape of platelets during infection has remained unexplored.

Conclusion

Taken together, this investigation provides the first exploration of the profound impact of infection on the human platelet lipidome, and reveals associations between the lipid composition of platelets and their reactivity. These results warrant further lipidomic research in other infections and disease states involving platelet pathophysiology.

Methods

We performed untargeted lipidomics in platelets of 25 patients hospitalized for COVID-19 and 23 noninfectious controls with similar age and sex characteristics, and with comparable comorbidities.

Objective

To investigate the platelet lipidome of patients hospitalized for COVID-19.

Results

Twenty-five percent of the 1,650 annotated lipids were significantly different between the groups. The significantly altered part of the platelet lipidome mostly comprised lipids that were less abundant in patients with COVID-19 (20.4% down, 4.6% up, 75% unchanged). Platelets from COVID-19 patients showed decreased levels of membrane plasmalogens, and a distinct decrease of long-chain, unsaturated triacylglycerols. Conversely, platelets from patients with COVID-19 displayed class-wide higher abundances of bis(monoacylglycero)phosphate and its biosynthetic precursor lysophosphatidylglycerol. Levels of these classes positively correlated with ex vivo platelet reactivity-as measured by P-selectin expression after PAR1 activation-irrespective of disease state.

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