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钙微区与氧化应激

Calcium microdomains and oxidative stress.

作者信息

Davidson Sean M, Duchen Michael R

机构信息

The Hatter Cardiovascular Institute, Royal Free and University College Medical School, London, Department of Medicine, 67 Chenies Mews, London, UK.

出版信息

Cell Calcium. 2006 Nov-Dec;40(5-6):561-74. doi: 10.1016/j.ceca.2006.08.017. Epub 2006 Oct 17.

Abstract

The phenomenon of calcium microdomains is firmly established in the field of subcellular physiology. These regions of localized, transient calcium increase are exemplified by the spontaneous 'sparks' released through the ryanodine receptor in myocytes, but include subplasmalemmal microdomains, focal calcium oscillations and microdomains enclosed within organelles, such as the endoplasmic reticulum, golgi and mitochondria. Increasing evidence suggests that oxidative stress regulates both the formation and disappearance of microdomains. Calcium release channels and transporters are all modulated by redox state, while several mechanisms that generate oxidative or nitrosative stress are regulated by calcium. Here, we discuss the evidence for the regulation of calcium microdomains by redox state, and, by way of example, demonstrate that the frequency of calcium sparks in cardiomyocytes is increased in response to oxidative stress. We consider the evidence for the existence of analogous microdomains of reactive oxygen and nitrogen species and suggest that the refinement of imaging techniques for these species might lead to similar concepts. The interaction between Ca(2+) microdomains and proteins that modulate their formation results in a complex and dynamic, spatial signaling mechanism, which is likely to be broadly applicable to different cell types, adding new dimensions to the calcium signaling 'toolkit'.

摘要

钙微区现象在亚细胞生理学领域已得到充分证实。这些局部性、短暂性钙增加的区域,以心肌细胞中通过兰尼碱受体释放的自发性“钙火花”为典型例子,但还包括质膜下微区、局部钙振荡以及细胞器(如内质网、高尔基体和线粒体)内的微区。越来越多的证据表明,氧化应激调节着微区的形成和消失。钙释放通道和转运体均受氧化还原状态的调节,而产生氧化或亚硝化应激的几种机制则受钙的调节。在此,我们讨论氧化还原状态调节钙微区的证据,并举例说明心肌细胞中钙火花的频率会因氧化应激而增加。我们考虑了活性氧和氮物种类似微区存在的证据,并提出针对这些物种成像技术的改进可能会产生类似的概念。Ca(2+)微区与调节其形成的蛋白质之间的相互作用导致了一种复杂而动态的空间信号传导机制,这可能广泛适用于不同细胞类型,为钙信号“工具包”增添了新的维度。

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