Salt‐inducible kinases are required for glucose uptake and insulin signaling in human adipocytes

Abstract

AbstractObjectiveSalt‐inducible kinase 2 (SIK2) is abundantly expressed in adipocytes and downregulated in adipose tissue from individuals with obesity or insulin resistance. The main aims of this work were to investigate the involvement of SIKs in the regulation of glucose uptake in primary mature human adipocytes and to identify mechanisms underlying this regulation.MethodsPrimary mature adipocytes were isolated from human, rat, or mouse adipose tissue and treated with pan‐SIK inhibitors. Adipocytes isolated from wild type, ob/ob, and SIK2 knockout mice were also used. Glucose uptake was examined by glucose tracer assay. The insulin signaling pathway was monitored by Western blotting, co‐immunoprecipitation, and total internal reflection fluorescence microscopy.ResultsThis study demonstrates that SIK2 is downregulated in obese ob/ob mice and that SIK activity is required for intact glucose uptake in primary human and mouse adipocytes. The underlying mechanism involves direct effects on the insulin signaling pathway, likely at the level of phosphatidylinositol (3,4,5)‐trisphosphate (PIP3) generation or breakdown. Moreover, lack of SIK2 alone is sufficient to attenuate glucose uptake in mouse adipocytes.ConclusionsSIK2 is required for insulin action in human adipocytes, and the mechanism includes direct effects on the insulin signaling pathway.