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蛋白质组学策略揭示骨骼肌与年龄相关的氧化还原信号缺陷。

Proteomic strategies to unravel age-related redox signalling defects in skeletal muscle.

机构信息

Free Radical Laboratory, Departments of Diabetes and Cardiovascular Sciences, Centre for Health Sciences, University of the Highlands and Islands, Inverness IV2 3JH, UK.

Oxford Innovation for Science and Technology Limited, Oxford OX4 2JY, UK.

出版信息

Free Radic Biol Med. 2019 Feb 20;132:24-32. doi: 10.1016/j.freeradbiomed.2018.09.012. Epub 2018 Sep 13.

Abstract

Increased oxidative damage and disrupted redox signalling are consistently associated with age-related loss of skeletal muscle mass and function. Redox signalling can directly regulate biogenesis and degradation pathways and indirectly via activation of key transcription factors. Contracting skeletal muscle fibres endogenously generate free radicals (e.g. superoxide) and non-radical derivatives (e.g. hydrogen peroxide). Exercise induced redox signalling can promote beneficial adaptive responses that are disrupted by age-related redox changes. Identifying and quantifying the redox signalling pathways responsible for successful adaptation to exercise makes skeletal muscle an attractive physiological model for redox proteomic approaches. Site specific identification of the redox modification and quantification of site occupancy in the context of protein abundance remains a crucial concept for redox proteomics approaches. Notwithstanding, the technical limitations associated with skeletal muscle for proteomic analysis, we discuss current approaches for the identification and quantification of transient and stable redox modifications that have been employed to date in ageing research. We also discuss recent developments in proteomic approaches in skeletal muscle and potential implications and opportunities for investigating disrupted redox signalling in skeletal muscle ageing.

摘要

氧化损伤增加和氧化还原信号紊乱与与年龄相关的骨骼肌质量和功能丧失密切相关。氧化还原信号可以直接调节生物发生和降解途径,并通过激活关键转录因子间接调节。收缩的骨骼肌纤维内源性地产生自由基(如超氧化物)和非自由基衍生物(如过氧化氢)。运动引起的氧化还原信号可以促进有益的适应性反应,但会被与年龄相关的氧化还原变化所破坏。确定和量化负责成功适应运动的氧化还原信号通路,使骨骼肌成为氧化还原蛋白质组学方法的有吸引力的生理模型。在蛋白质丰度的背景下,对氧化还原修饰的特异性定位和对位点占有率的定量仍然是氧化还原蛋白质组学方法的关键概念。尽管如此,与骨骼肌进行蛋白质组学分析相关的技术限制,我们将讨论目前用于鉴定和量化瞬时和稳定氧化还原修饰的方法,这些方法迄今为止已被用于衰老研究。我们还讨论了骨骼肌蛋白质组学方法的最新进展,以及调查骨骼肌衰老中氧化还原信号紊乱的潜在意义和机会。

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