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对影响小鼠眼晶状体白内障形成的蛋白质的鉴定。

Identification of proteins that modify cataract of mouse eye lens.

作者信息

Hoehenwarter Wolfgang, Tang Yajun, Ackermann Renate, Pleissner Klaus-Peter, Schmid Monika, Stein Robert, Zimny-Arndt Ursula, Kumar Nalin M, Jungblut Peter R

机构信息

Max Planck Institute for Infection Biology, Core Facility Protein Analysis, Berlin, Germany.

出版信息

Proteomics. 2008 Dec;8(23-24):5011-24. doi: 10.1002/pmic.200800380.

Abstract

The occurrence of a nuclear cataract in the eye lens due to disruption of the alpha3Cx46 connexin gene, Gja3, is dependent on strain background in a mouse model, implicating factors that modify the pathology. The differences upon cataractogenesis in the urea soluble proteins of the lens of two mouse strains, C57BL/6J and 129/SvJ, were analyzed by a comparative proteomics approach. Determination of the complete proteome of an organ offers the opportunity to characterize at a molecular level, differences in gene expression and PTMs occurring during pathology and between individuals. The abundance of 63 protein species was altered between the strains. A unique aspect of this study is the identification of chaperonin subunit 6A, mortalin, ERp29, and syntaxin-binding protein 6 in the eye lens. DNA polymorphisms resulting in nonconservative amino acid changes that led to altered physicochemical properties of the proteins were detected for mortalin, chaperonin subunit 6A, annexin A1, and possibly gamma-N crystallin. The results show HSP27/25 and/or ERp29 are the likely major modifying factors for cataractogenesis. Extension of the results suggests that small heat-shock proteins have a major role for influencing cataract formation in humans.

摘要

在小鼠模型中,由于α3Cx46连接蛋白基因Gja3的破坏,晶状体中核性白内障的发生取决于品系背景,这暗示了修饰病理过程的因素。采用比较蛋白质组学方法分析了两种小鼠品系C57BL/6J和129/SvJ晶状体中尿素可溶性蛋白质在白内障发生过程中的差异。确定一个器官的完整蛋白质组提供了在分子水平上表征病理过程中以及个体之间基因表达和翻译后修饰差异的机会。品系间63种蛋白质的丰度发生了改变。这项研究的一个独特之处在于在晶状体中鉴定出伴侣蛋白亚基6A、mortalin、ERp29和Syntaxin结合蛋白6。检测到导致非保守氨基酸变化从而导致蛋白质理化性质改变的DNA多态性,涉及mortalin、伴侣蛋白亚基6A、膜联蛋白A1以及可能的γ-N晶状体蛋白。结果表明HSP27/25和/或ERp29可能是白内障发生的主要修饰因子。结果的拓展表明,小热休克蛋白在影响人类白内障形成中起主要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/51fa/3018240/4940ca47c231/nihms250132f1.jpg

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