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Peroxisome Proliferator-Activated Receptor Delta: A Conserved Director of Lipid Homeostasis through Regulation of the Oxidative Capacity of Muscle

机译:过氧化物酶体增殖物激活的受体三角洲:通过调节肌肉的氧化能力的脂质稳态的保守主任。

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摘要

The peroxisome proliferator-activated receptors (PPARs), which are ligand-inducible transcription factors expressed in a variety of tissues, have been shown to perform key roles in lipid homeostasis. In physiological situations such as fasting and physical exercise, one PPAR subtype, PPARδ, triggers a transcriptional program in skeletal muscle leading to a switch in fuel usage from glucose/fatty acids to solely fatty acids, thereby drastically increasing its oxidative capacity. The metabolic action of PPARδ has also been verified in humans. In addition, it has become clear that the action of PPARδ is not restricted to skeletal muscle. Indeed, PPARδ has been shown to play a crucial role in whole-body lipid homeostasis as well as in insulin sensitivity, and it is active not only in skeletal muscle (as an activator of fat burning) but also in the liver (where it can activate glycolysis/lipogenesis, with the produced fat being oxidized in muscle) and in the adipose tissue (by incrementing lipolysis). The main aim of this review is to highlight the central role for activated PPARδ in the reversal of any tendency toward the development of insulin resistance.
机译:过氧化物酶体增殖物激活受体(PPAR)是在多种组织中表达的配体诱导转录因子,已显示在脂质体内平衡中起关键作用。在诸如禁食和体育锻炼等生理情况下,一种PPAR亚型PPARδ触发骨骼肌中的转录程序,从而导致燃料使用量从葡萄糖/脂肪酸转换为仅脂肪酸,从而大大提高了其氧化能力。 PPARδ的代谢作用也已在人体中得到证实。另外,已经清楚的是,PPARδ的作用不限于骨骼肌。确实,PPARδ已被证明在全身脂质稳态和胰岛素敏感性中起着至关重要的作用,它不仅在骨骼肌(作为脂肪燃烧的激活剂)中起作用,而且在肝脏中(它可以激活糖酵解/脂肪生成,产生的脂肪在肌肉和脂肪组织中被氧化(通过增加脂解作用)。这篇综述的主要目的是强调激活的PPARδ在逆转任何胰岛素抵抗发展趋势中的核心作用。

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