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氧化应激和蛋白质氧化在衰老过程中的作用。

Role of oxidative stress and protein oxidation in the aging process.

作者信息

Sohal Rajindar S

机构信息

Department of Molecular Pharmacology and Toxicology, University of Southern California, Los Angeles, CA 90033, USA.

出版信息

Free Radic Biol Med. 2002 Jul 1;33(1):37-44. doi: 10.1016/s0891-5849(02)00856-0.

Abstract

The hypothesis is that the rate of oxygen consumption and the ensuing accrual of molecular oxidative damage constitute a fundamental mechanism governing the rate of aging is supported by several lines of evidence: (i) life spans of cold blooded animals and mammals with unstable basal metabolic rate (BMR) are extended and oxidative damage (OxD) is attenuated by an experimental decrease in metabolic rate; (ii) single gene mutations in Drosophila and Caenorhabditis elegans that extend life span almost invariably result in a generalized slowing of physiological activities, albeit via different mechanisms, affecting a decrease in OxD; (iii) caloric restriction decreases body temperature and OxD; and, (iv) results of studies on the effects of transgenic overexpressions of antioxidant enzymes are generally supportive, but quite ambiguous. It is suggested that oxidative damage to proteins plays a crucial role in aging because oxidized proteins lose catalytic function and are preferentially hydrolyzed. It is hypothesized that oxidative damage to specific proteins constitutes one of the mechanisms linking oxidative stress/damage and age-associated losses in physiological functions.

摘要

以下证据支持了这一假说

即氧气消耗率以及随之产生的分子氧化损伤累积构成了控制衰老速率的一种基本机制:(i)基础代谢率(BMR)不稳定的冷血动物和哺乳动物,其寿命会因实验性代谢率降低而延长,氧化损伤(OxD)也会减轻;(ii)果蝇和秀丽隐杆线虫中的单基因突变延长了寿命,几乎无一例外会导致生理活动普遍减缓,尽管其机制不同,但都会使氧化损伤减少;(iii)热量限制会降低体温和氧化损伤;以及(iv)关于抗氧化酶转基因过表达效应的研究结果总体上是支持性的,但相当模糊。有人提出,蛋白质的氧化损伤在衰老过程中起关键作用,因为氧化的蛋白质会失去催化功能并优先被水解。据推测,特定蛋白质的氧化损伤构成了将氧化应激/损伤与生理功能的年龄相关丧失联系起来的机制之一。

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