A selective inhibitor of ceramide synthase 1 reveals a novel role in fat metabolism.
Nigel TurnerXin Ying LimHamish D ToopBrenna OsborneAmanda E BrandonElysha N TaylorCorrine E FiveashHemna GovindarajuJonathan D TeoHolly P McEwenTimothy A CouttasStephen M ButlerAbhirup DasGreg M KowalskiClinton R BruceKyle Lee HoehnThomas FathCarsten Schmitz-PeifferGregory J CooneyMagdalene K MontgomeryJonathan C MorrisAnthony S DonPublished in: Nature communications (2018)
Specific forms of the lipid ceramide, synthesized by the ceramide synthase enzyme family, are believed to regulate metabolic physiology. Genetic mouse models have established C16 ceramide as a driver of insulin resistance in liver and adipose tissue. C18 ceramide, synthesized by ceramide synthase 1 (CerS1), is abundant in skeletal muscle and suggested to promote insulin resistance in humans. We herein describe the first isoform-specific ceramide synthase inhibitor, P053, which inhibits CerS1 with nanomolar potency. Lipidomic profiling shows that P053 is highly selective for CerS1. Daily P053 administration to mice fed a high-fat diet (HFD) increases fatty acid oxidation in skeletal muscle and impedes increases in muscle triglycerides and adiposity, but does not protect against HFD-induced insulin resistance. Our inhibitor therefore allowed us to define a role for CerS1 as an endogenous inhibitor of mitochondrial fatty acid oxidation in muscle and regulator of whole-body adiposity.
Keyphrases
- insulin resistance
- high fat diet
- skeletal muscle
- adipose tissue
- fatty acid
- high fat diet induced
- polycystic ovary syndrome
- metabolic syndrome
- type diabetes
- glycemic control
- physical activity
- oxidative stress
- weight gain
- transcription factor
- single cell
- hydrogen peroxide
- endothelial cells
- diabetic rats
- weight loss
- copy number