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Practical guide for dynamic monitoring of protein oxidation using genetically encoded ratiometric fluorescent biosensors of methionine sulfoxide

机译:使用遗传编码的甲硫醇亚硫氧化物的遗传编码比荧光生物传感器动态监测蛋白质氧化的实用指南

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In cells, physiological and pathophysiological conditions may lead to the formation of methionine sulfoxide (MetO). This oxidative modification of methionine exists in the form of two diastereomers, R and S, and may occur in both free amino acid and proteins. MetO is reduced back to methionine by methionine sulfoxide reductases (MSRs). Methionine oxidation was thought to be a nonspecific modification affecting protein functions and methionine availability. However, recent findings suggest that cyclic methionine oxidation and reduction is a posttranslational modification that actively regulates protein function akin to redox regulation by cysteine oxidation and phosphorylation. Methionine oxidation is thus an important mechanism that could play out in various physiological contexts. However, detecting MetO generation and MSR functions remains challenging because of the lack of tools and reagents to detect and quantify this protein modification. We recently developed two genetically encoded diasterospecific fluorescent sensors, MetSOx and MetROx, to dynamically monitor MetO in living cells. Here, we provide a detailed procedure for their use in bacterial and mammalian cells using fluorimetric and fluorescent imaging approaches. This method can be adapted to dynamically monitor methionine oxidation in various cell types and under various conditions. (C) 2016 Elsevier Inc. All rights reserved.
机译:在细胞中,生理和病理生理病症可能导致形成甲硫氨酸硫氧化物(Meto)。这种蛋氨酸的氧化改性以两种非对映异构体,R和S的形式存在,并且可以在游离氨基酸和蛋白质中发生。通过甲硫氨酸硫氧化物还原酶(MSRS)减少回到甲硫氨酸。认为甲硫氨酸氧化是影响蛋白质功能和蛋氨酸可用性的非特异性修饰。然而,最近的发现表明,循环甲硫氨酸氧化和还原是一种后期改性,其通过半胱氨酸氧化和磷酸化,积极调节蛋白质功能类似于氧化还原调节的蛋白质功能。因此,甲硫氨酸氧化是可以在各种生理环境中发挥作用的重要机制。然而,由于缺乏检测和量化该蛋白质改性,检测emo代和MSR功能仍然具有挑战性。我们最近开发了两种遗传编码的基因型荧光传感器,梅索克斯和Metrox,以动态监测活细胞中的eCO。在这里,我们提供了使用荧光和荧光成像方法在细菌和哺乳动物细胞中使用的详细程序。该方法可以适于在各种细胞类型和各种条件下动态监测甲硫氨酸氧化。 (c)2016年Elsevier Inc.保留所有权利。

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