Inflammatory pathways and insulin action.

G S Hotamisligil
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引用次数: 715

Abstract

Obesity and type 2 diabetes are associated with a state of abnormal inflammatory response. While this correlation has also been recognized in the clinical setting, its molecular basis and physiological significance are not yet fully understood. Studies in recent years have provided important insights into this curious phenomenon. The state of chronic inflammation typical of obesity and type 2 diabetes occurs at metabolically relevant sites, such as the liver, muscle, and most interestingly, adipose tissues. The biological relevance of the activation of inflammatory pathways became evident upon the demonstration that interference with these pathways improve or alleviate insulin resistance. The abnormal production of tumor necrosis factor alpha (TNF-alpha) in obesity is a paradigm for the metabolic significance of this inflammatory response. When TNF-alpha activity is blocked in obesity, either biochemically or genetically, the result is improved insulin sensitivity. Studies have since focused on the identification of additional inflammatory mediators critical in metabolic control and on understanding the molecular mechanisms by which inflammatory pathways are coupled to metabolic control. Recent years have seen a critical progress in this respect by the identification of several downstream mediators and signaling pathways, which provide the crosstalk between inflammatory and metabolic signaling. These include the discovery of c-Jun N-terminal kinase (JNK) and I kappa beta kinase (I kappa K) as critical regulators of insulin action activated by TNF-alpha and other inflammatory and stress signals, and the identification of potential targets. Here, the role of the JNK pathway in insulin receptor signaling, the impact of blocking this pathway in obesity and the mechanisms underlying JNK-induced insulin resistance will be discussed.

炎症途径和胰岛素作用。
肥胖和2型糖尿病与异常炎症反应状态相关。虽然这种相关性在临床环境中也得到了认可,但其分子基础和生理意义尚未完全了解。近年来的研究为这一奇怪的现象提供了重要的见解。肥胖和2型糖尿病典型的慢性炎症状态发生在代谢相关部位,如肝脏、肌肉和最有趣的脂肪组织。炎症途径激活的生物学相关性在证明干扰这些途径可改善或减轻胰岛素抵抗后变得明显。肥胖中肿瘤坏死因子α (tnf - α)的异常产生是这种炎症反应代谢意义的一个范例。当肥胖患者体内的tnf - α活性被生化或基因阻断时,胰岛素敏感性就会得到改善。从那以后,研究的重点是鉴定在代谢控制中起关键作用的其他炎症介质,以及了解炎症途径与代谢控制耦合的分子机制。近年来,通过鉴定几种下游介质和信号通路,在这方面取得了关键进展,这些介质和信号通路提供了炎症和代谢信号之间的串扰。其中包括发现c-Jun n -末端激酶(JNK)和I kappa β激酶(I kappa K)是由tnf - α和其他炎症和应激信号激活的胰岛素作用的关键调节因子,并确定潜在靶点。本文将讨论JNK通路在胰岛素受体信号传导中的作用、阻断该通路对肥胖的影响以及JNK诱导胰岛素抵抗的机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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