Platelets Release Mitochondrial Antigens in Systemic Lupus Erythematosus

Overview

Journal Sci Transl Med

Specialties General Medicine
Science

Date 2021 Feb 18

PMID 33597264

Citations 35

Authors

Imene Melki

Isabelle Allaeys

Nicolas Tessandier

Tania Levesque

Nathalie Cloutier

Audree Laroche

Nathalie Vernoux

Yann Becker

Hadrien Benk-Fortin

Anne Zufferey

Emmanuelle Rollet-Labelle

Marc Pouliot

Guy Poirier

Natacha Patey

Clemence Belleannee

Denis Soulet

Steven E McKenzie

Alain Brisson

Marie-Eve Tremblay

Christian Lood

Paul R Fortin

Eric Boilard

Affiliations

Soon will be listed here.

Abstract

The accumulation of DNA and nuclear components in blood and their recognition by autoantibodies play a central role in the pathophysiology of systemic lupus erythematosus (SLE). Despite the efforts, the sources of circulating autoantigens in SLE are still unclear. Here, we show that in SLE, platelets release mitochondrial DNA, the majority of which is associated with the extracellular mitochondrial organelle. Mitochondrial release in patients with SLE correlates with platelet degranulation. This process requires the stimulation of platelet FcγRIIA, a receptor for immune complexes. Because mice lack FcγRIIA and murine platelets are completely devoid of receptor capable of binding IgG-containing immune complexes, we used transgenic mice expressing FcγRIIA for our in vivo investigations. FcγRIIA expression in lupus-prone mice led to the recruitment of platelets in kidneys and to the release of mitochondria in vivo. Using a reporter mouse with red fluorescent protein targeted to the mitochondrion, we confirmed platelets as a source of extracellular mitochondria driven by FcγRIIA and its cosignaling by the fibrinogen receptor α2bβ3 in vivo. These findings suggest that platelets might be a key source of mitochondrial antigens in SLE and might be a therapeutic target for treating SLE.

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