展开性视网膜营养不良：分子伴侣的作用？

Unfolding retinal dystrophies: a role for molecular chaperones?

作者信息

Chapple J P, Grayson C, Hardcastle A J, Saliba R S, van der Spuy J, Cheetham M E

机构信息

Dept of Pathology, Institute of Ophthalmology, University College London, 11-43 Bath Street, London, UK EC1V 9EL.

出版信息

Trends Mol Med. 2001 Sep;7(9):414-21. doi: 10.1016/s1471-4914(01)02103-7.

DOI:10.1016/s1471-4914(01)02103-7

PMID:11530337

Abstract

Inherited retinal dystrophy is a major cause of blindness worldwide. Recent molecular studies have suggested that protein folding and molecular chaperones might play a major role in the pathogenesis of these degenerations. Incorrect protein folding could be a common consequence of causative mutations in retinal degeneration disease genes, particularly mutations in the visual pigment rhodopsin. Furthermore, several retinal degeneration disease genes have recently been identified as putative facilitators of correct protein folding, molecular chaperones, on the basis of sequence homology. We also consider whether manipulation of chaperone levels or chaperone function might offer potential novel therapies for retinal degeneration.

摘要

遗传性视网膜营养不良是全球失明的主要原因。最近的分子研究表明，蛋白质折叠和分子伴侣可能在这些退行性病变的发病机制中起主要作用。错误的蛋白质折叠可能是视网膜退行性疾病基因致病突变的常见后果，尤其是视觉色素视紫红质中的突变。此外，基于序列同源性，最近已鉴定出几种视网膜退行性疾病基因是正确蛋白质折叠的假定促进因子，即分子伴侣。我们还考虑了操纵伴侣蛋白水平或伴侣蛋白功能是否可能为视网膜退行性变提供潜在的新疗法。

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展开性视网膜营养不良：分子伴侣的作用？

Unfolding retinal dystrophies: a role for molecular chaperones?

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