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CLC氯离子通道与转运体:生物物理学与生理学视角

CLC chloride channels and transporters: a biophysical and physiological perspective.

作者信息

Zifarelli G, Pusch M

机构信息

CNR, Istituto di Biofisica, Via De Marini 6, 16149 Genova, Italy.

出版信息

Rev Physiol Biochem Pharmacol. 2007;158:23-76. doi: 10.1007/112_2006_0605.

Abstract

Chloride-transporting proteins play fundamental roles in many tissues in the plasma membrane as well as in intracellular membranes. They have received increasing attention in the last years because crucial, and often unexpected and novel, physiological functions have been disclosed with gene-targeting approaches, X-ray crystallography, and biophysical analysis. CLC proteins form a gene family that comprises nine members in mammals, at least four of which are involved in human genetic diseases. The X-ray structure of the bacterial CLC homolog, ClC-ec1, revealed a complex fold and confirmed the anticipated homodimeric double-barreled architecture of CLC-proteins with two separate Cl-ion transport pathways, one in each subunit. Four of the mammalian CLC proteins, ClC-1, ClC-2, ClC-Ka, and ClC-Kb, are chloride ion channels that fulfill their functional roles-stabilization of the membrane potential, transepithelial salt transport, and ion homeostasisin the plasma membrane. The other five CLC proteins are predominantly expressed in intracellular organelles like endosomes and lysosomes, where they are probably important for a proper luminal acidification, in concert with the V-type H+-ATPase. Surprisingly, ClC-4, ClC-5, and probably also ClC-3, are not Cl- ion channels but exhibit significant Cl-/H+ antiporter activity, as does the bacterial homolog ClC-ec1 and the plant homolog AtCLCa. The physiological significance of the Cl-/H+ antiport activity remains to be established.

摘要

氯离子转运蛋白在质膜以及细胞内膜的许多组织中发挥着重要作用。在过去几年中,它们受到了越来越多的关注,因为通过基因靶向方法、X射线晶体学和生物物理分析揭示了关键的、往往意想不到的新生理功能。CLC蛋白形成一个基因家族,在哺乳动物中包括九个成员,其中至少有四个与人类遗传疾病有关。细菌CLC同源物ClC-ec1的X射线结构揭示了一种复杂的折叠,并证实了CLC蛋白预期的同型二聚体双桶结构,有两条独立的氯离子运输途径,每个亚基各有一条。四种哺乳动物CLC蛋白,即ClC-1、ClC-2、ClC-Ka和ClC-Kb,是氯离子通道,它们在质膜中发挥其功能作用——稳定膜电位、跨上皮盐运输和离子稳态。其他五种CLC蛋白主要在内体和溶酶体等细胞内细胞器中表达,在那里它们可能与V型H⁺-ATP酶协同作用,对管腔的适当酸化很重要。令人惊讶的是,ClC-4、ClC-5,可能还有ClC-3,不是氯离子通道,而是表现出显著的Cl⁻/H⁺反向转运活性,细菌同源物ClC-ec1和植物同源物AtCLCa也是如此。Cl⁻/H⁺反向转运活性的生理意义尚待确定。

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