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蛋白质中的 3-硝基酪氨酸和相关衍生物:前体、自由基中间体及其对功能的影响。

3-Nitrotyrosine and related derivatives in proteins: precursors, radical intermediates and impact in function.

机构信息

Departamento de Bioquímica, Facultad de Medicina, Universidad de la República, Montevideo, Uruguay.

Centro de Investigaciones Biomédicas (CEINBIO), Universidad de la República, Montevideo, Uruguay.

出版信息

Essays Biochem. 2020 Feb 17;64(1):111-133. doi: 10.1042/EBC20190052.

Abstract

Oxidative post-translational modification of proteins by molecular oxygen (O2)- and nitric oxide (•NO)-derived reactive species is a usual process that occurs in mammalian tissues under both physiological and pathological conditions and can exert either regulatory or cytotoxic effects. Although the side chain of several amino acids is prone to experience oxidative modifications, tyrosine residues are one of the preferred targets of one-electron oxidants, given the ability of their phenolic side chain to undergo reversible one-electron oxidation to the relatively stable tyrosyl radical. Naturally occurring as reversible catalytic intermediates at the active site of a variety of enzymes, tyrosyl radicals can also lead to the formation of several stable oxidative products through radical-radical reactions, as is the case of 3-nitrotyrosine (NO2Tyr). The formation of NO2Tyr mainly occurs through the fast reaction between the tyrosyl radical and nitrogen dioxide (•NO2). One of the key endogenous nitrating agents is peroxynitrite (ONOO-), the product of the reaction of superoxide radical (O2•-) with •NO, but ONOO--independent mechanisms of nitration have been also disclosed. This chemical modification notably affects the physicochemical properties of tyrosine residues and because of this, it can have a remarkable impact on protein structure and function, both in vitro and in vivo. Although low amounts of NO2Tyr are detected under basal conditions, significantly increased levels are found at pathological states related with an overproduction of reactive species, such as cardiovascular and neurodegenerative diseases, inflammation and aging. While NO2Tyr is a well-established stable oxidative stress biomarker and a good predictor of disease progression, its role as a pathogenic mediator has been laboriously defined for just a small number of nitrated proteins and awaits further studies.

摘要

蛋白质的氧化后翻译修饰是一个普遍的过程,由分子氧(O2)和一氧化氮(•NO)衍生的活性物质在生理和病理条件下发生在哺乳动物组织中,可以发挥调节或细胞毒性作用。虽然几个氨基酸的侧链容易经历氧化修饰,但酪氨酸残基是一电子氧化剂的首选靶标之一,因为其酚侧链能够经历可逆的单电子氧化,形成相对稳定的酪氨酸自由基。酪氨酸自由基作为各种酶活性部位的天然可逆催化中间体,也可以通过自由基-自由基反应导致几种稳定的氧化产物的形成,如 3-硝基酪氨酸(NO2Tyr)。NO2Tyr 的形成主要通过酪氨酸自由基和二氧化氮(•NO2)之间的快速反应发生。一种关键的内源性硝化剂是过氧亚硝酸盐(ONOO-),是超氧自由基(O2•-)与•NO 反应的产物,但也揭示了 ONOO--独立的硝化机制。这种化学修饰显著影响酪氨酸残基的物理化学性质,因此,它可以对蛋白质结构和功能产生显著影响,无论是在体外还是体内。虽然在基础条件下检测到少量的 NO2Tyr,但在与活性物质过度产生相关的病理状态下,如心血管和神经退行性疾病、炎症和衰老,发现其水平显著增加。虽然 NO2Tyr 是一种公认的稳定氧化应激生物标志物,也是疾病进展的良好预测指标,但作为一种致病介质的作用仅在少数硝化蛋白中得到了艰难的定义,还需要进一步的研究。

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