Hepatic deletion of Mboat7 (LPIAT1) causes activation of SREBP-1c and fatty liver

Genetic variants that increase the risk of fatty liver disease and cirrhosis have recently been identified in the proximity of membrane-bound O -acyltransferase domain-containing 7 ( MBOAT7 ). To elucidate the link between these variants and fatty liver disease, we characterized Mboat7 liver-specific KO mice ( Mboat7 LSKO). Chow-fed Mboat7 LSKO mice developed fatty livers and associated liver injury. Lipidomic analysis of liver using MS revealed a pronounced reduction in 20-carbon PUFA content in phosphatidylinositols (PIs) but not in other phospholipids. The change in fatty acid composition of PIs in these mice was associated with a marked increase in de novo lipogenesis because of activation of SREBP-1c, a transcription factor that coordinates the activation of genes encoding enzymes in the fatty acid biosynthesis pathway. Hepatic removal of both SREBP cleavage-activating protein ( Scap ) and Mboat7 normalized hepatic triglycerides relative to Scap -only hepatic KO, showing that increased SREBP-1c processing is required for Mboat7 -induced steatosis. This study reveals a clear relationship between PI fatty acid composition and regulation of hepatic fat synthesis and delineates the mechanism by which mutations in MBOAT7 cause hepatic steatosis.