Abstract

Systemic lupus erythematosus (SLE) is an autoimmune disease characterized by defective regulatory T (T_reg) cells. Here, we demonstrate that a T cell-specific deletion of calcium/calmodulin-dependent protein kinase 4 (CaMK4) improves disease in B6.<i>lpr</i> lupus-prone mice and expands T_reg cells. Mechanistically, CaMK4 phosphorylates the glycolysis rate-limiting enzyme 6-phosphofructokinase, platelet type (PFKP) and promotes aerobic glycolysis, while its end product fructose-1,6-biphosphate suppresses oxidative metabolism. In T_reg cells, a CRISPR-Cas9-enabled <i>Pfkp</i> deletion recapitulated the metabolism of <i>Camk4</i>^-/- T_reg cells and improved their function and stability in vitro and in vivo. In SLE CD4⁺ T cells, PFKP enzymatic activity correlated with SLE disease activity and pharmacologic inhibition of CaMK4-normalized PFKP activity, leading to enhanced T_reg cell function. In conclusion, we provide molecular insights in the defective metabolism and function of T_reg cells in SLE and identify PFKP as a target to fine-tune T_reg cell metabolism and thereby restore their function.