Boyden Penelope A, Davies Sean S, Viswanathan Prakash C, Amarnath Venkataraman, Balser Jeffrey R, Roberts L Jackson
Department of Pharmacology, Columbia University College of Physicians and Surgeons, New York, NY 10032, USA.
J Cardiovasc Pharmacol. 2007 Nov;50(5):480-6. doi: 10.1097/FJC.0b013e31815a0564.
Unabated reactive oxygen species (ROS) are potentiated by an ischemia-induced shift in anaerobic metabolism, which generates superoxide anion upon reperfusion and reintroduction of oxygen. ROS can modify protein structure and function in fundamental ways, one of which is by forming reactive lipid species from the oxidation of lipids. In this review, we discuss these pathways and discuss the literature that shows that these species can produce dramatic effects on cardiac ion channel function (eg, Na+ channel function). Furthermore, we review what is known about the generation of such in the highly remodeled post myocardial infarction substrate. We suggest prevention of adduction of these highly reactive compounds would be antiarrhythmic.
缺血诱导的无氧代谢转变会增强未减弱的活性氧(ROS),这种转变在再灌注和重新引入氧气时会产生超氧阴离子。ROS可以从根本上改变蛋白质的结构和功能,其中一种方式是通过脂质氧化形成反应性脂质物种。在本综述中,我们讨论了这些途径,并讨论了相关文献,这些文献表明这些物种可对心脏离子通道功能(如Na+通道功能)产生显著影响。此外,我们回顾了在高度重塑的心肌梗死后基质中此类物质产生的已知情况。我们认为预防这些高反应性化合物的内收将具有抗心律失常作用。
Zotero 插件