Abstract |
Dissecting the pathways regulating the adaptive immune response in atherosclerosis is of particular therapeutic interest. Here we report that the lipid G-protein coupled receptor GPR55 is highly expressed by splenic plasma cells (PC), upregulated in mouse spleens during atherogenesis and human unstable or ruptured compared to stable plaques. Gpr55-deficient mice developed larger atherosclerotic plaques with increased necrotic core size compared to their corresponding controls. Lack of GPR55 hyperactivated B cells, disturbed PC maturation and resulted in immunoglobulin (Ig)G overproduction. B cell-specific Gpr55 depletion or adoptive transfer of Gpr55-deficient B cells was sufficient to promote plaque development and elevated IgG titers. In vitro, the endogenous GPR55 ligand lysophsophatidylinositol (LPI) enhanced PC proliferation, whereas GPR55 antagonism blocked PC maturation and increased their mitochondrial content. Collectively, these discoveries provide previously undefined evidence for GPR55 in B cells as a key modulator of the adaptive immune response in atherosclerosis.
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Authors | Raquel Guillamat-Prats, Daniel Hering, Abhishek Derle, Martina Rami, Carmen Härdtner, Donato Santovito, Petteri Rinne, Laura Bindila, Michael Hristov, Sabrina Pagano, Nicolas Vuilleumier, Sofie Schmid, Aleksandar Janjic, Wolfgang Enard, Christian Weber, Lars Maegdefessel, Alexander Faussner, Ingo Hilgendorf, Sabine Steffens |
Journal | Nature cardiovascular research
(Nat Cardiovasc Res)
Vol. 1
Pg. 1056-1071
(Nov 2022)
ISSN: 2731-0590 [Electronic] England |
PMID | 36523570
(Publication Type: Journal Article)
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