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首页> 外文期刊>Diabetes >Paradoxical Coupling of Triglyceride Synthesis and Fatty Acid Oxidation in Skeletal Muscle Overexpressing DGAT1
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Paradoxical Coupling of Triglyceride Synthesis and Fatty Acid Oxidation in Skeletal Muscle Overexpressing DGAT1

机译:甘油三酸酯过表达DGAT1的甘油三酸酯合成和脂肪酸氧化的悖论耦合。

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OBJECTIVE: Transgenic expression of diacylglycerol acyltransferase-1 (DGAT1) in skeletal muscle leads to protection against fat-induced insulin resistance despite accumulation of intramuscular triglyceride, a phenomenon similar to what is known as the "athlete paradox." The primary objective of this study is to determine how DGAT1 affects muscle fatty acid oxidation in relation to whole-body energy metabolism and insulin sensitivity. RESEARCH DESIGN AND METHODS: We first quantified insulin sensitivity and the relative tissue contributions to the improved whole-body insulin sensitivity in muscle creatine kisase (MCK)-DGAT1 transgenic mice by hyperinsulinemic-euglycemic clamps. Metabolic consequences of DGAT1 overexpression in skeletal muscles were determined by quantifying triglyceride synthesis/storage (anabolic) and fatty acid oxidation (catabolic), in conjunction with gene expression levels of representative marker genes in fatty acid metabolism. Whole-body energy metabolism including food consumption, body weights, oxygen consumption, locomotor activity, and respiration exchange ratios were determined at steady states. RESULTS: MCK-DGAT1 mice were protected against muscle lipoptoxicity, although they remain susceptible to hepatic lipotoxicity. While augmenting triglyceride synthesis, DGAT1 overexpression also led to increased muscle mitochondrial fatty acid oxidation efficiency, as compared with wild-type muscles. On a high-fat diet, MCK-DGAT1 mice displayed higher basal metabolic rates and 5-10% lower body weights compared with wild-type littermates, whereas food consumption was not different. CONCLUSIONS: DGAT1 overexpression in skeletal muscle led to parallel increases in triglyceride synthesis and fatty acid oxidation. Seemingly paradoxical, this phenomenon is characteristic of insulin-sensitive myofibers and suggests that DGAT1 plays an active role in metabolic "remodeling" of skeletal muscle coupled with insulin sensitization.
机译:目的:尽管肌内甘油三酸酯蓄积,骨骼肌中二酰基甘油酰基转移酶-1(DGAT1)的转基因表达可防止脂肪诱导的胰岛素抵抗,这种现象类似于所谓的“运动员悖论”。这项研究的主要目的是确定DGAT1与全身能量代谢和胰岛素敏感性有关如何影响肌肉脂肪酸氧化。研究设计和方法:我们首先通过高胰岛素-正常血糖钳夹定量了肌酸肌酸激酶(MCK)-DGAT1转基因小鼠的胰岛素敏感性及其对改善全身胰岛素敏感性的相关组织贡献。 DGAT1在骨骼肌中过表达的代谢结果是通过量化甘油三酸酯的合成/存储(合成代谢)和脂肪酸氧化(分解代谢)以及脂肪酸代谢中代表性标记基因的基因表达水平来确定的。在稳态下确定全身能量代谢,包括食物消耗,体重,氧气消耗,运动能力和呼吸交换率。结果:尽管MCK-DGAT1小鼠仍然易受肝脂毒性的影响,但它们具有抗肌肉脂毒性的保护作用。与野生型肌肉相比,在增加甘油三酸酯合成的同时,DGAT1的过表达还导致肌肉线粒体脂肪酸氧化效率提高。在高脂饮食中,与野生型同窝仔相比,MCK-DGAT1小鼠显示出更高的基础代谢率和较低的体重5-10%,而食物消耗没有差异。结论:骨骼肌中DGAT1的过表达导致甘油三酸酯合成和脂肪酸氧化的平行增加。似乎矛盾的是,这种现象是胰岛素敏感性肌纤维的特征,表明DGAT1在骨骼肌的代谢“重塑”以及胰岛素敏感性中起积极作用。

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  • 来源
    《Diabetes》 |2009年第11期|p.2516-2524|共9页
  • 作者

    Li Liu Xiaojing Shi Cheol Soo Choi Gerald I Shulman Katherine Klaus K Sreekumaran Nair Gary J Schwartz Yiying Zhang Ira J Goldberg Yi-Hao Yu;

  • 作者单位

    Li Liu,1 Xiaojing Shi,1 Cheol Soo Choi,2 Gerald I. Shulman,2 Katherine Klaus,3 K. Sreekumaran Nair,3 Gary J. Schwartz,4 Yiying Zhang,5 Ira J. Goldberg,1 and Yi-Hao Yu1From the 1 Department of Medicine. Preventive Medicine and Nutrition. Columbia University. New York, New York: the 2 Departments of Internal Medicine and Cellular and Molecular Physiology, Howard Hughes Medical Institute. Yale University School of Medicine, New Haven. Connecticut, the 3 Endocrine Research Unit and Department of Laboratory Meditine. Mayo Clinic College of Medicine, Rochester, Minnesota, the 'Department of Medicine & Neuroscience. Diabetes Research and Training Center. Albert Einstein College of Medicine. New York. New York: and the 'Department of Pediatrics. Naomi Berrie Diabetes Center. Columbia University, New York. New York.Corresponding author Yi-Hao Yu. yy102@columbia.edu.Received 11 August 2008 and accepted 16 July 2009. Published ahead of print at http://diabetes.diabetesjournals.org on 12 August 2009. DOl: 10.2337/ db08-1096.C.S.C. is currently affiliated with the Laboratory of Cellular & Molecular Physiology and Metabolism, Lee Gil Ya Cancer and Diabetes Institute. Gachon University of Medicine and Science, Incheon, Korea.© 2009 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work Ls not altered. See http://crealivecommons.org/licenses/by -nc-nd/3.0/ for details.The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked "advertisement" in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.,;

  • 收录信息 美国《科学引文索引》(SCI);美国《化学文摘》(CA);
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  • 入库时间 2022-08-17 13:45:51

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