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Intracellular localization of diacylglycerols and sphingolipids influences insulin sensitivity and mitochondrial function in human skeletal muscle

机译:二酰基甘油和鞘脂的细胞内定位影响人体骨骼肌的胰岛素敏感性和线粒体功能

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>BACKGROUND. Accumulation of diacylglycerol (DAG) and sphingolipids is thought to promote skeletal muscle insulin resistance by altering cellular signaling specific to their location. However,the subcellular localization of bioactive lipids in human skeletal muscle is largely unknown.>METHODS. We evaluated subcellular localization of skeletal muscle DAGs and sphingolipids in lean individuals (n = 15), endurance-trained athletes (n = 16), and obese men and women with (n = 12) and without type 2 diabetes (n = 15). Muscle biopsies were fractionated into sarcolemmal, cytosolic, mitochondrial/ER, and nuclear compartments. Lipids were measured using liquid chromatography tandem mass spectrometry, and insulin sensitivity was measured using hyperinsulinemic-euglycemic clamp.>RESULTS. Sarcolemmal 1,2-DAGs were not significantly related to insulin sensitivity. Sarcolemmal ceramides were inversely related to insulin sensitivity, with a significant relationship found for the C18:0 species. Sarcolemmal sphingomyelins were also inversely related to insulin sensitivity, with the strongest relationships found for the C18:1, C18:0, and C18:2 species. In the mitochondrial/ER and nuclear fractions, 1,2-DAGs were positively related to, while ceramides were inversely related to, insulin sensitivity. Cytosolic lipids as well as 1,3-DAG, dihydroceramides, and glucosylceramides in any compartment were not related to insulin sensitivity. All sphingolipids but only specific DAGs administered to isolated mitochondria decreased mitochondrial state 3 respiration.>CONCLUSION. These data reveal previously unknown differences in subcellular localization of skeletal muscle DAGs and sphingolipids that relate to whole-body insulin sensitivity and mitochondrial function in humans. These data suggest that whole-cell concentrations of lipids obscure meaningful differences in compartmentalization and suggest that subcellular localization of lipids should be considered when developing therapeutic interventions to treat insulin resistance.>FUNDING. National Institutes of Health General Clinical Research Center (RR-00036), National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK) (R01DK089170), NIDDK (T32 DK07658), and Colorado Nutrition Obesity Research Center (P30DK048520).
机译:>背景。人们认为,二酰基甘油(DAG)和鞘脂的积累可通过改变特定于其位置的细胞信号传导来促进骨骼肌胰岛素抵抗。但是,人体骨骼肌中生物活性脂质的亚细胞定位仍然是未知的。 = 16),肥胖男性和女性(n = 12),且没有2型糖尿病(n = 15)。将肌肉活检分为肌膜,胞质,线粒体/ ER和核区室。用液相色谱串联质谱法测定脂质,用高胰岛素-正常血糖钳夹法测定胰岛素敏感性。>结果。肌膜上的1,2-DAG与胰岛素敏感性无显着相关性。肌膜神经酰胺与胰岛素敏感性呈负相关,与C18:0物种之间存在显着关系。肌膜鞘磷脂也与胰岛素敏感性成反比,与C18:1,C18:0和C18:2种类的关系最密切。在线粒体/ ER和核部分中,1,2-DAG与胰岛素敏感性呈正相关,而神经酰胺与胰岛素敏感性呈负相关。任何隔室中的细胞脂质以及1,3-DAG,二氢神经酰胺和葡萄糖基神经酰胺均与胰岛素敏感性无关。所有的鞘脂,但只有特定的DAG给予分离的线粒体,才能降低线粒体3状态的呼吸。在人类中发挥作用。这些数据表明脂质的全细胞浓度掩盖了区室的有意义的差异,并建议在开发治疗措施来治疗胰岛素抵抗时应考虑脂质的亚细胞定位。>资金。中心(RR-00036),美国糖尿病与消化与肾脏疾病研究所(NIDDK)(R01DK089170),NIDDK(T32 DK07658)和科罗拉多州营养肥胖症研究中心(P30DK048520)。

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