Mitochondrial complex II in intestinal epithelial cells regulates T cell-mediated immunopathology.
Hideaki FujiwaraKeisuke SeikeMichael D BrooksAnna V MathewIlya KovalenkoAnupama PalHo-Joon LeeDaniel PeltierStephanie KimChen LiuKatherine Oravecz-WilsonLu LiYaping SunJaeman ByunYoshinobu MaedaMax S WichaThomas L SaundersAlnawaz RehemtullaCostas Andreas LyssiotisSubramaniam PennathurPavan ReddyPublished in: Nature immunology (2021)
Intestinal epithelial cell (IEC) damage by T cells contributes to graft-versus-host disease, inflammatory bowel disease and immune checkpoint blockade-mediated colitis. But little is known about the target cell-intrinsic features that affect disease severity. Here we identified disruption of oxidative phosphorylation and an increase in succinate levels in the IECs from several distinct in vivo models of T cell-mediated colitis. Metabolic flux studies, complemented by imaging and protein analyses, identified disruption of IEC-intrinsic succinate dehydrogenase A (SDHA), a component of mitochondrial complex II, in causing these metabolic alterations. The relevance of IEC-intrinsic SDHA in mediating disease severity was confirmed by complementary chemical and genetic experimental approaches and validated in human clinical samples. These data identify a critical role for the alteration of the IEC-specific mitochondrial complex II component SDHA in the regulation of the severity of T cell-mediated intestinal diseases.