Article ID | Journal | Published Year | Pages | File Type |
---|---|---|---|---|
1949048 | Biochimica et Biophysica Acta (BBA) - Molecular and Cell Biology of Lipids | 2016 | 15 Pages |
Abstract
Sphingomyelin synthase 2 (SMS2) is a proposed potential therapeutic target for obesity and insulin resistance. However, the contributions of SMS2 to glucose metabolism in tissues and its possible therapeutic mechanisms remain unclear. Thus, to determine whole-body glucose utilization and the contributions of each insulin-targeted tissue to glucose uptake, we performed a glucose kinetics study, using the radiolabeled glucose analog 18F-2-fluoro-2-deoxy-D-glucose (18F-FDG), in wild-type (WT) and SMS2 knockout (KO) mice. Insulin signaling was enhanced in the liver, white adipose tissue and skeletal muscle of SMS2 KO mice compared with those of WT mice. In addition, compared with in WT mice, blood clearance of 18F-FDG was accelerated in SMS2 KO mice when they were fed either a normal or a high fat diet. 18F-FDG uptake was also increased in insulin-targeted tissues such as skeletal muscle in the SMS2 KO mice. Whereas skeletal muscle sphingolipid content was not clearly affected, plasma levels of very long-chain fatty acid (VLCFA)-containing ceramides were markedly increased in SMS2 KO mice, compared with in WT mice. We also generated liver-conditional SMS2 KO mice and performed glucose and insulin tolerance tests on mice with a high fat diet. However, no significant effect was observed. Thus, our study provided evidence that genetic inhibition of SMS2 elevated glucose clearance through activation of glucose uptake into insulin-targeted tissues such as skeletal muscle by a mechanism independent of hepatic SMS2. Our findings further indicate that this occurs, at least in part, via indirect mechanisms such as elevation of VLCFA-containing ceramides.
Keywords
VLCFAHFDGastrocnemiusALTS1PIBATGLUT18F-FDGOGTTGAPDHFFAPET-CTT2DMNEFAIRβinsulin receptor β subunitSPINMACerSHOMA-RGSIShexosylceramideIL-6SPLSdhCerHexCerAUCquadriceps femorisH&ELC/ESI-MS/MSinsulin tolerance testOral glucose tolerance testASTAspartate aminotransferaseAlanine aminotransferaseHomeostasis model assessment-insulin resistancesphingolipidssphingomyelinSphingosine 1 phosphatesphingomyelin synthaseFree fatty acidVery long-chain fatty acidNon-esterified fatty acidFatty acid oxidationinterleukin-6ITTquatriacylglycerolpositron emission tomography-computed tomographyGlucose uptakeGlucose transporterDihydroceramideType 2 diabetes mellitusDiaphragmdiacylglycerolDIAHigh fat dietnormal dietembryonic stemCerceramideSolceramide synthaseSoleusendoplasmic reticulumFAOInsulin resistanceknockoutwild-typeHematoxylin and Eosinpolymerase chain reactionPCRSMSWATtotal-cholesterolGasGluGluteus maximusglyceraldehyde-3-phosphate dehydrogenase
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Authors
Masayuki Sugimoto, Yoichi Shimizu, Songji Zhao, Naoyuki Ukon, Ken-ichi Nishijima, Masato Wakabayashi, Takeshi Yoshioka, Kenichi Higashino, Yoshito Numata, Tomohiko Okuda, Nagara Tamaki, Hisatoshi Hanamatsu, Yasuyuki Igarashi, Yuji Kuge,