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[氯离子通道蛋白(ClC型)的多种功能]

[Various functions of ClC-type Cl- channels].

作者信息

Furukawa Tetsushi

机构信息

Department of Bio-informational Pharmacology, Medical Research Institute, Tokyo Medical and Dental University, Japan.

出版信息

Nihon Yakurigaku Zasshi. 2003 Nov;122(5):375-83. doi: 10.1254/fpj.122.375.

Abstract

Cellular functions of Cl- channels are poorly understood, in contrast to well-established roles of cation channels. Recently, important achievements in Cl- channel research have been sequentially reported, including cloning of many Cl- channel cDNAs, linkage of gene abnormalities to human inherited disorders, analysis of knock-out mouse phenotype, analysis of crystal structure, and regulation by protein-protein interaction. Intracellular membrane Cl- channels are important for acidification of intracellular vesicles: ClC-5 functions for re-absorption of low-molecular-weight proteins in renal proximal tubule, and ClC-7 for absorption of bone matrix by osteoclasts. Abnormal functions of these channels result in Dent's disease characterized by proteinuria and kidney stones and by osteopetrosis, respectively. Plasma membrane Cl- channels, ClC-K1, ClC-K2, and ClC-3B, are expressed predominantly in epithelial cells and are important for uni-directional Cl- transport across the epithelia. Abnormalities of these channels are also related to human diseases: abnormal ClC-K1 to diabetes insipidus and abnormal ClC-K2 to Bartter's syndrome.

摘要

与阳离子通道已明确的作用相比,人们对氯离子通道的细胞功能了解甚少。最近,氯离子通道研究陆续取得了重要成果,包括克隆出许多氯离子通道的cDNA、将基因异常与人类遗传性疾病联系起来、分析基因敲除小鼠的表型、分析晶体结构以及蛋白质 - 蛋白质相互作用的调节。细胞内膜氯离子通道对于细胞内囊泡的酸化很重要:ClC - 5在肾近端小管中负责重吸收低分子量蛋白质,而ClC - 7则参与破骨细胞对骨基质的吸收。这些通道的功能异常分别导致以蛋白尿和肾结石为特征的丹特病以及骨质石化症。质膜氯离子通道ClC - K1、ClC - K2和ClC - 3B主要在上皮细胞中表达,对于氯离子跨上皮细胞的单向转运很重要。这些通道的异常也与人类疾病有关:ClC - K1异常与尿崩症有关,ClC - K2异常与巴特综合征有关。

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