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肾脏氯离子通道与氯化钠转运的关系。

Renal Chloride Channels in Relation to Sodium Chloride Transport.

机构信息

Sorbonne Université, CNRS, INSERM, Centre de recherche des Cordeliers, Equipe Métabolisme et Physiologie Rénale, Paris, France.

Centro de Estudios Científicos, Valdivia, Chile.

出版信息

Compr Physiol. 2018 Dec 13;9(1):301-342. doi: 10.1002/cphy.c180024.

DOI:10.1002/cphy.c180024
PMID:30549019
Abstract

The many mechanisms governing NaCl absorption in the diverse parts of the renal tubule have been largely elucidated, although some of them, as neutral NaCl absorption across the cortical collecting duct or regulation through with-no-lysine (WNK) kinases have emerged only recently. Chloride channels, which are important players in these processes, at least in the distal nephron, are the focus of this review. Over the last 20-year period, experimental studies using molecular, electrophysiological, and physiological/functional approaches have deepened and renewed our views on chloride channels and their role in renal function. Two chloride channels of the ClC family, named as ClC-Ka and ClC-Kb in humans and ClC-K1 and ClC-K2 in other mammals, are preponderant and play complementary roles: ClC-K1/Ka is mainly involved in the building of the interstitial cortico-medullary concentration gradient, while ClC-K2/Kb participates in NaCl absorption in the thick ascending limb, distal convoluted tubule and the intercalated cells of the collecting duct. The two ClC-Ks might also be involved indirectly in proton secretion by type A intercalated cells. Other chloride channels in the kidneys include CFTR, TMEM16A, and probably volume-regulated LRRC8 chloride channels, whose function and molecular identity have not as yet been established. © 2019 American Physiological Society. Compr Physiol 9:301-342, 2019.

摘要

尽管调控肾单位不同部位 NaCl 吸收的多种机制已经基本阐明,但其中一些机制,如皮质集合管中中性 NaCl 的吸收或通过无赖氨酸(WNK)激酶的调节,直到最近才被发现。氯离子通道在这些过程中是重要的参与者,至少在远曲小管中是如此。在过去的 20 年中,使用分子、电生理和生理/功能方法的实验研究加深并更新了我们对氯离子通道及其在肾功能中的作用的认识。ClC 家族的两种氯离子通道,在人类中命名为 ClC-Ka 和 ClC-Kb,在其他哺乳动物中命名为 ClC-K1 和 ClC-K2,它们占主导地位并发挥互补作用:ClC-K1/Ka 主要参与建立间质皮质-髓质浓度梯度,而 ClC-K2/Kb 参与在升支粗段、远曲小管和集合管闰细胞中的 NaCl 吸收。这两种 ClC-Ks 也可能间接地参与 A 型闰细胞的质子分泌。肾脏中的其他氯离子通道包括 CFTR、TMEM16A,可能还有体积调节的 LRRC8 氯离子通道,其功能和分子特性尚未确定。 2019 年美国生理学会。综合生理学 9:301-342, 2019.

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