内质网的卫士和罪魁祸首:II型糖尿病的糖脂毒性和β细胞衰竭。

Experimental Diabetes Research Pub Date : 2012-01-01 Epub Date: 2011-10-01 DOI:10.1155/2012/639762
Udayakumar Karunakaran, Han-Jong Kim, Joon-Young Kim, In-Kyu Lee
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引用次数: 42

摘要

内质网(ER)是一种细胞器,负责多种重要的细胞功能,包括用于分泌的新合成蛋白质的生物合成和折叠,如胰岛素。内质网参与新陈代谢的所有分支,将营养感知与细胞信号传导联系起来。许多病理和生理因素干扰内质网功能,诱发内质网应激。内质网应激触发适应性信号级联反应,称为未折叠蛋白反应(UPR),以缓解应激。UPR不能解决内质网应激导致病理状况,如β细胞功能障碍和死亡,以及II型糖尿病。然而,对于内质网对高血糖(糖毒性)、高脂血症(脂毒性)以及两者联合(糖脂毒性)反应的控制和调节的细节知之甚少。本文考虑了最近关于如何调节反应的见解,这可能为糖脂中毒诱导的II型糖尿病进展过程中内质网应激介导的β细胞功能障碍和死亡机制提供线索。
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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Guards and culprits in the endoplasmic reticulum: glucolipotoxicity and β-cell failure in type II diabetes.

The endoplasmic reticulum (ER) is a cellular organelle responsible for multiple important cellular functions including the biosynthesis and folding of newly synthesized proteins destined for secretion, such as insulin. The ER participates in all branches of metabolism, linking nutrient sensing to cellular signaling. Many pathological and physiological factors perturb ER function and induce ER stress. ER stress triggers an adaptive signaling cascade, called the unfolded protein response (UPR), to relieve the stress. The failure of the UPR to resolve ER stress leads to pathological conditions such as β-cell dysfunction and death, and type II diabetes. However, much less is known about the fine details of the control and regulation of the ER response to hyperglycemia (glucotoxicity), hyperlipidemia (lipotoxicity), and the combination of both (glucolipotoxicity). This paper considers recent insights into how the response is regulated, which may provide clues into the mechanism of ER stress-mediated β-cell dysfunction and death during the progression of glucolipotoxicity-induced type II diabetes.

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来源期刊
Experimental Diabetes Research
Experimental Diabetes Research 医学-内分泌学与代谢
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