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线粒体活性氧以及Bcl-2作为线粒体活性氧调节因子的作用

Mitochondrial ROS and involvement of Bcl-2 as a mitochondrial ROS regulator.

作者信息

Chong Stephen Jun Fei, Low Ivan Cherh Chiet, Pervaiz Shazib

机构信息

Department of Physiology, Yong Loo Lin School of Medicine, National University of Singapore, 10 Medical Drive, Clinical Research Center, #04-25, Singapore 117597, Singapore.

Department of Physiology, Yong Loo Lin School of Medicine, National University of Singapore, 10 Medical Drive, Clinical Research Center, #04-25, Singapore 117597, Singapore; NUS Graduate School for Integrative Sciences and Engineering, Centre for Life Sciences (CeLS), #05-01, 28 Medical Drive, Singapore 117576, Singapore; Cancer and Stem Cell Biology Program, Duke-NUS Graduate Medical School, Singapore; Singapore-MIT Alliance, Singapore; National University Cancer Institute, Singapore.

出版信息

Mitochondrion. 2014 Nov;19 Pt A:39-48. doi: 10.1016/j.mito.2014.06.002. Epub 2014 Jun 19.

Abstract

Mitochondria are the major intracellular source of reactive oxygen species (ROS). While excessive mitochondrial ROS (mitoROS) production induces cell injury and death, there is accumulating evidence that non-toxic low levels of mitoROS could serve as important signaling molecules. Therefore, maintenance of mitoROS at physiological levels is crucial for cell homeostasis as well as for survival and proliferation. This review describes the various mechanisms that keep mitoROS in check, with particular focus on the role of the onco-protein Bcl-2 in redox regulation. In addition to its canonical anti-apoptotic activity, Bcl-2 has been implicated in mitoROS regulation by its effect on mitochondrial complex IV activity, facilitating the mitochondrial incorporation of GSH and interaction with the small GTPase-Rac1 at the mitochondria. We also discuss some of the plausible mechanism(s) which allows Bcl-2 to sense and respond to the fluctuations in mitoROS.

摘要

线粒体是细胞内活性氧(ROS)的主要来源。虽然过量的线粒体ROS(mitoROS)生成会诱导细胞损伤和死亡,但越来越多的证据表明,无毒的低水平mitoROS可作为重要的信号分子。因此,将mitoROS维持在生理水平对于细胞稳态以及生存和增殖至关重要。本综述描述了控制mitoROS的各种机制,特别关注癌蛋白Bcl-2在氧化还原调节中的作用。除了其典型的抗凋亡活性外,Bcl-2还通过其对线粒体复合物IV活性的影响、促进线粒体谷胱甘肽的掺入以及在线粒体与小GTP酶-Rac1的相互作用,参与了mitoROS的调节。我们还讨论了一些可能使Bcl-2感知并响应mitoROS波动的机制。

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