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数据非依赖采集蛋白质组学揭示急性肾损伤期间线粒体和过氧化物酶体蛋白的显著下调

Substantial Downregulation of Mitochondrial and Peroxisomal Proteins during Acute Kidney Injury revealed by Data-Independent Acquisition Proteomics.

作者信息

Burton Jordan B, Silva-Barbosa Anne, Bons Joanna, Rose Jacob, Pfister Katherine, Simona Fabia, Gandhi Tejas, Reiter Lukas, Bernhardt Oliver, Hunter Christie L, Goetzman Eric S, Sims-Lucas Sunder, Schilling Birgit

出版信息

bioRxiv. 2023 Feb 26:2023.02.26.530107. doi: 10.1101/2023.02.26.530107.

DOI:10.1101/2023.02.26.530107
PMID:36865241
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9980295/
Abstract

Acute kidney injury (AKI) manifests as a major health concern, particularly for the elderly. Understanding AKI-related proteome changes is critical for prevention and development of novel therapeutics to recover kidney function and to mitigate the susceptibility for recurrent AKI or development of chronic kidney disease. In this study, mouse kidneys were subjected to ischemia-reperfusion injury, and the contralateral kidneys remained uninjured to enable comparison and assess injury-induced changes in the kidney proteome. A fast-acquisition rate ZenoTOF 7600 mass spectrometer was introduced for data-independent acquisition (DIA) for comprehensive protein identification and quantification. Short microflow gradients and the generation of a deep kidney-specific spectral library allowed for high-throughput, comprehensive protein quantification. Upon AKI, the kidney proteome was completely remodeled, and over half of the 3,945 quantified protein groups changed significantly. Downregulated proteins in the injured kidney were involved in energy production, including numerous peroxisomal matrix proteins that function in fatty acid oxidation, such as ACOX1, CAT, EHHADH, ACOT4, ACOT8, and Scp2. Injured mice exhibited severely declined health. The comprehensive and sensitive kidney-specific DIA assays highlighted here feature high-throughput analytical capabilities to achieve deep coverage of the kidney proteome and will serve as useful tools for developing novel therapeutics to remediate kidney function.

摘要

急性肾损伤(AKI)是一个重大的健康问题,尤其是对老年人而言。了解与AKI相关的蛋白质组变化对于预防和开发恢复肾功能以及降低复发性AKI或慢性肾病易感性的新型疗法至关重要。在本研究中,对小鼠肾脏进行缺血再灌注损伤,对侧肾脏保持未损伤状态,以便进行比较并评估损伤诱导的肾脏蛋白质组变化。引入了快速采集速率的ZenoTOF 7600质谱仪进行数据非依赖采集(DIA),以进行全面的蛋白质鉴定和定量。短微流梯度和深度肾脏特异性光谱库的生成实现了高通量、全面的蛋白质定量。发生AKI时,肾脏蛋白质组完全重塑,3945个定量蛋白质组中有超过一半发生了显著变化。受损肾脏中下调的蛋白质参与能量产生,包括许多在脂肪酸氧化中起作用的过氧化物酶体基质蛋白,如ACOX1、CAT、EHHADH、ACOT4、ACOT8和Scp2。受损小鼠的健康状况严重下降。这里重点介绍的全面且灵敏的肾脏特异性DIA检测方法具有高通量分析能力,可实现对肾脏蛋白质组的深度覆盖,并将成为开发恢复肾功能新型疗法的有用工具。