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• W1655135214 abstract "Abstract Autoreactive CD4 T cells are key effectors in Systemic Lupus Erythematosus (SLE). Cell metabolism is an important checkpoint for T cell activation, proliferation, and differentiation. We hypothesized that 1) SLE T cells have metabolic defects that cause abnormal T cell functions; 2) Targeting T cell metabolism may abrogate T cell inflammatory functions and reduce disease symptoms in SLE mice. Metabolism of CD4 T cells from lupus-resistant B6 mice and the congenic lupus model B6.Sle1.Sle2.Sle3 (B6.TC) were studied. Here it was observed that compared to B6, CD4 T cells from B6.TC mice have a stronger glycolysis and a higher mitochondrial oxygen consumption, as well as an enhanced mTOR activity. To normalize T cell metabolism in B6.TC mice, we used metformin, which activates the AMPK pathway and inhibits mitochondrial oxygen consumption, and 2-DG, an inhibitor of glycolysis. In vitro, metformin blocks IFNγ production by CD4 T cells and facilitates Treg development. 2-DG also blocks IFNγ production, but only after T cell activation. In vivo, a combined treatment with metformin and 2-DG of B6.TC mice normalized T cell metabolism and reversed disease phenotypes, including T cell activation and autoantibody production. Further, CD4 T cells from SLE patients have an enhanced metabolism as compared to healthy controls, and excessive IFNγ production was significantly reduced by metformin. Our research suggests that T cell metabolism is a novel target for SLE treatment." @default.
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• W1655135214 date "2014-05-01" @default.
• W1655135214 modified "2023-09-27" @default.
• W1655135214 title "Metabolic inhibitors normalize CD4 T cell metabolism and functions, and reverse disease in a murine model of lupus (THER5P.839)" @default.
• W1655135214 doi "https://doi.org/10.4049/jimmunol.192.supp.200.18" @default.
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