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首页> 外文期刊>Diabetes >Lipid-Induced Insulin Resistance Affects Women Less Than Men and Is Not Accompanied by Inflammation or Impaired Proximal Insulin Signaling
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Lipid-Induced Insulin Resistance Affects Women Less Than Men and Is Not Accompanied by Inflammation or Impaired Proximal Insulin Signaling

机译:脂质诱导的胰岛素抵抗比男性少影响女性,并且不伴有炎症或近端胰岛素信号传导受损

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摘要

Objective-we have previously shown that overnight fasted women have higher insulin-stimulated whole body and leg glucose uptake despite a higher intramyocellular triacylglycerol concentration than men. Women also express higher muscle mrna levels of proteins related to lipid metabolism than men. We therefore hypothesized that women would be less prone to lipid-induced insulin resistance. Research design and methods-insulin sensitivity of whole-body and leg glucose disposal was studied in 16 young well-matched healthy men and women infused with intralipid or saline for 7 h. Muscle biopsies were obtained before and during a euglycemic-hyperinsulinemic clamp (1.42 mu • kg~(-1)• min ~1). Results-intralipid infusion reduced whole-body glucose infusion rate by 26% in women and 38% in men (p < 0.05), and insulin-stimulated leg glucose uptake was reduced significantly less in women (45%) than men (60%) after intralipid infusion. Hepatic glucose production was decreased during the clamp similarly in women and men irrespective of intralipid infusion. Intralipid did not impair insulin or ampk signaling in muscle and subcutaneous fat, did not cause accumulation of muscle lipid intermediates, and did not impair insulin-stimulated glycogen synthase activity in muscle or increase plasma concentrations of inflammatory cytokines. In vitro glucose transport in giant sar-colemmal vesicles was not decreased by acute exposure to fatty acids. Leg lactate release was increased and respiratory exchange ratio was decreased by intralipid. Conclusions-intralipid infusion causes less insulin resistance of muscle glucose uptake in women than in men. This insulin resistance is not due to decreased canonical insulin signaling, accumulation of lipid intermediates, inflammation, or direct inhibition of glut activity. Rather, a higher leg lactate release and lower glucose oxidation with intralipid infusion may suggest a metabolic feedback regulation of glucose metabolism. Diabetes 60:64-73, 2011
机译:我们以前的目标研究表明,尽管肌细胞内三酰基甘油的浓度高于男性,但过夜禁食的妇女体内胰岛素刺激的全身和腿部葡萄糖摄入量较高。与男性相比,女性还表现出更高的与脂质代谢有关的蛋白质,其肌肉mRNA含量更高。因此,我们假设妇女将不太容易受到脂质诱导的胰岛素抵抗。研究设计和方法-在16名健康状况良好的年轻男性和女性中注入脂质或盐水7小时,研究了全身胰岛素和小腿葡萄糖处置的敏感性。在正常血糖-高胰岛素钳夹之前和期间进行肌肉活检(1.42μ•kg〜(-1)•min〜1)。结果-脂质体内输注使女性的全身葡萄糖输注率降低了26%,男性降低了38%(p <0.05),胰岛素刺激的腿部葡萄糖摄取的降低率明显低于女性(45%),低于男性(60%)脂质内输注后。不论是否输注脂质,男女在钳夹过程中肝葡萄糖的产生均类似地下降。脂质体内不会损害肌肉和皮下脂肪中的胰岛素或ampk信号传导,不会引起肌肉脂质中间体的积聚,也不会损害肌肉中胰岛素刺激的糖原合酶活性或增加炎症细胞因子的血浆浓度。急性暴露于脂肪酸并不会降低巨大的肌膜-小囊泡中的体外葡萄糖运输。脂质内使腿部乳酸释放增加,呼吸交换率降低。结论脂质体内输注导致女性的肌肉葡萄糖摄取胰岛素抵抗比男性少。这种胰岛素抵抗不是由于规范的胰岛素信号传导减少,脂质中间体的积累,炎症或对谷氨酰胺活性的直接抑制所致。相反,较高的腿部乳酸释放和较低的脂质内输注葡萄糖氧化可能表明对葡萄糖代谢的代谢反馈调节。糖尿病60:64-73,2011

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  • 来源
    《Diabetes》 |2011年第1期|p.63-72|共10页
  • 作者

    Louise D. H0eg; Kim A. Sj0berg; Jacob Jeppesen; Thomas E. Jensen; Christian Frosig; Jesper B. Birk; Bruno Bisiani; Natalie Hiscock; Henriette Pilegaard; J0rgen F.P. Wojtaszewski; Erik A. Richter; Bente Kiens;

  • 作者单位

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

    Unilever Discover,Colworth Science Park, Sharnbrook, Bedfordshire, U.K.;

    Copenhagen Muscle Research Centre, Department of Molecular Biology, University of Copenhagen, and the Centre of Inflammation and Metabolism,Copenhagen, Denmark;

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

    Copenhagen Muscle Research Centre, Molecular Physiology Group,Section of Human Physiology, Department of Exercise and Sport Sciences,University of Copenhagen, Copenhagen, Denmark;

  • 收录信息 美国《科学引文索引》(SCI);美国《化学文摘》(CA);
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  • 正文语种 eng
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  • 入库时间 2022-08-18 03:46:32

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