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Skeletal Muscle–Specific Deletion of Lipoprotein Lipase Enhances Insulin Signaling in Skeletal Muscle but Causes Insulin Resistance in Liver and Other Tissues

机译：骨骼肌特定的脂蛋白脂肪酶的缺失增强骨骼肌中的胰岛素信号传导但导致肝脏和其他组织的胰岛素抵抗

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>OBJECTIVE—Skeletal muscle–specific LPL knockout mouse (SMLPL^−/−) were created to study the systemic impact of reduced lipoprotein lipid delivery in skeletal muscle on insulin sensitivity, body weight, and composition.>RESEARCH DESIGN AND METHODS—Tissue-specific insulin sensitivity was assessed using a hyperinsulinemic-euglycemic clamp and 2-deoxyglucose uptake. Gene expression and insulin-signaling molecules were compared in skeletal muscle and liver of SMLPL^−/− and control mice.>RESULTS—Nine-week-old SMLPL^−/− mice showed no differences in body weight, fat mass, or whole-body insulin sensitivity, but older SMLPL^−/− mice had greater weight gain and whole-body insulin resistance. High-fat diet feeding accelerated the development of obesity. In young SMLPL^−/− mice, insulin-stimulated glucose uptake was increased 58% in the skeletal muscle, but was reduced in white adipose tissue (WAT) and heart. Insulin action was also diminished in liver: 40% suppression of hepatic glucose production in SMLPL^−/− vs. 90% in control mice. Skeletal muscle triglyceride was 38% lower, and insulin-stimulated phosphorylated Akt (Ser473) was twofold greater in SMLPL^−/− mice without changes in IRS-1 tyrosine phosphorylation and phosphatidylinositol 3-kinase activity. Hepatic triglyceride and liver X receptor, carbohydrate response element–binding protein, and PEPCK mRNAs were unaffected in SMLPL^−/− mice, but peroxisome proliferator–activated receptor (PPAR)-γ coactivator-1α and interleukin-1β mRNAs were higher, and stearoyl–coenzyme A desaturase-1 and PPARγ mRNAs were reduced.>CONCLUSIONS—LPL deletion in skeletal muscle reduces lipid storage and increases insulin signaling in skeletal muscle without changes in body composition. Moreover, lack of LPL in skeletal muscle results in insulin resistance in other key metabolic tissues and ultimately leads to obesity and systemic insulin resistance.

机译：>目的— 创建骨骼肌特异性LPL基因敲除小鼠（SMLPL ^{-/-），以研究骨骼肌中脂蛋白脂质递送减少对胰岛素敏感性，体重的系统性影响>研究设计与方法— 使用高胰岛素-正常血糖钳夹和2-脱氧葡萄糖摄取评估组织特异性胰岛素敏感性。比较了SMLPL ^{-/-和对照组小鼠的骨骼肌和肝脏中的基因表达和胰岛素信号分子。>结果— 九周大的SMLPL ^{-/ − 小鼠的体重，脂肪量或全身胰岛素敏感性均无差异，但年龄较大的SMLPL ^{-/-小鼠具有更大的体重增加和全身胰岛素抵抗。高脂饮食喂养加速了肥胖的发展。在年轻的SMLPL ^{-/-小鼠中，骨骼肌中胰岛素刺激的葡萄糖摄取增加了58％，而白色脂肪组织（WAT）和心脏的摄取减少了。肝脏中的胰岛素作用也减弱了：SMLPL ^{-/-中抑制肝葡萄糖产生的比例为40％，而对照小鼠为90％。骨骼肌甘油三酸酯降低38％，胰岛素刺激的磷酸化Akt（Ser473）在SMLPL ^{-/-小鼠中增加两倍，而IRS-1酪氨酸磷酸化和磷脂酰肌醇3激酶活性没有变化。 SMLPL ^{-/-小鼠的肝甘油三酸酯和肝X受体，碳水化合物反应元件结合蛋白和PEPCK mRNA均未受到影响，但过氧化物酶体增殖物激活受体（PPAR）-γ共激活因子-1α和白介素- 1βmRNAs较高，而硬脂酰辅酶A去饱和酶1和PPARγmRNAs减少。>结论— 骨骼肌中LLP的缺失减少了脂质的储存并增加了骨骼肌中胰岛素的信号，而没有改变身体的组成。此外，骨骼肌缺乏LPL会导致其他关键代谢组织的胰岛素抵抗，最终导致肥胖和全身性胰岛素抵抗。}}}}}}}}

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期刊名称 Diabetes
作者
Hong Wang; Leslie A. Knaub; Dalan R. Jensen; Dae Young Jung; Eun-Gyoung Hong; Hwi-Jin Ko; Alison M. Coates; Ira J. Goldberg; Becky A. de la Houssaye; Rachel C. Janssen; Carrie E. McCurdy; Shaikh M. Rahman; Cheol Soo Choi; Gerald I. Shulman; Jason K. Kim; Jacob E. Friedman; Robert H. Eckel;
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年(卷),期 2009(58),1
年度 2009
页码 116–124
总页数 9
原文格式 PDF
正文语种
中图分类基础医学;
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专利

1. Skeletal Muscle-Specific Deletion of Lipoprotein Lipase Enhances Insulin Signaling in Skeletal Muscle but Causes Insulin Resistance in Liver and Other Tissues [J] . Hong Wang Leslie A Knaub Dalan R Jensen Dae Young Jung Eun-Gyoung Hong Hwi-Jin Ko Alison M Coates Ira J Goldberg Becky A de la Houssaye Rachel C Janssen Carrie E McCurdy Shaikh M Rahman Cheol Soo Choi Gerald I Shulman Jason K Kim Diabetes . 2009,第1期

机译：骨骼肌脂蛋白脂肪酶的特异性缺失可增强骨骼肌中的胰岛素信号传导，但会引起肝脏和其他组织的胰岛素抵抗
2. Skeletal Muscle-specific Deletion Of Lipoprotein Lipaseenhances Insulin Signaling In Skeletal Muscle But Causesrninsulin Resistance In Liver And Other Tissues [J] . Hong Wang, Leslie A. Knaub, Dalan R. Jensen, Diabetes . 2009,第1期

机译：骨骼肌脂蛋白脂肪酶的特异性缺失增强了骨骼肌中胰岛素的信号传导，但在肝脏和其他组织中引起了胰岛素抵抗
3. Skeletal Muscle-Specific Deletion of MKP-1 Reveals a p38 MAPK/JNK/Akt Signaling Node That Regulates Obesity-Induced Insulin Resistance [J] . Ahmed Lawan, Kisuk Min, Lei Zhang, Diabetes . 2018,第4期

机译：骨骼肌特定的MKP-1删除揭示了调节肥胖诱导的胰岛素抵抗的p38 MAPK / JNK / Akt信号转导节点。
4. Insulin signaling of glucose uptake in skeletal muscle of lactating dairy cows [C] . S.K. Spachmann, U. Schdnhusen, B. Kuhla, International Symposium on Energy and Protein Metabolism and Nutrition . 2013

机译：血糖摄取的胰岛素信号在哺乳奶牛骨骼肌中的血糖摄取
5. Effects of lower- and higher- volume resistance exercise on serum testosterone and skeletal muscle androgen receptor content in men: Subsequent effects on the mrna expression of insulin-like growth factor peptide and myostatin in skeletal muscle. [D] . Spillane, Mike. 2013

机译：较低和较高容量的抵抗运动对男性血清睾丸激素和骨骼肌雄激素受体含量的影响：随后对骨骼肌中胰岛素样生长因子肽和肌生成抑制素的mRNA表达的影响。
6. Skeletal Muscle–Specific Deletion of MKP-1 Reveals a p38 MAPK/JNK/Akt Signaling Node That Regulates Obesity-Induced Insulin Resistance [O] . Ahmed Lawan, Kisuk Min, Lei Zhang, 2018

机译：骨骼肌特异性MKP-1的缺失揭示了调节肥胖诱导的胰岛素抵抗的p38 MAPK / JNK / Akt信号传导节点
7. Skeletal Muscle–Specific Deletion of Lipoprotein Lipase Enhances Insulin Signaling in Skeletal Muscle but Causes Insulin Resistance in Liver and Other Tissues [O] . Wang, Hong, Knaub, Leslie A., Jensen, Dalan R., 2008

机译：骨骼肌脂蛋白脂肪酶的特异性缺失增强骨骼肌中胰岛素的信号传导，但导致肝脏和其他组织的胰岛素抵抗

Skeletal Muscle–Specific Deletion of Lipoprotein Lipase Enhances Insulin Signaling in Skeletal Muscle but Causes Insulin Resistance in Liver and Other Tissues

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