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紧密连接蛋白在髓袢升支粗段的镶嵌表达导致细胞旁钠离子和镁离子转运的空间分离。

Mosaic expression of claudins in thick ascending limbs of Henle results in spatial separation of paracellular Na+ and Mg2+ transport.

作者信息

Milatz Susanne, Himmerkus Nina, Wulfmeyer Vera Christine, Drewell Hoora, Mutig Kerim, Hou Jianghui, Breiderhoff Tilman, Müller Dominik, Fromm Michael, Bleich Markus, Günzel Dorothee

机构信息

Institute of Physiology, Christian-Albrechts-University of Kiel, 24098 Kiel, Germany;

Institute of Physiology, Christian-Albrechts-University of Kiel, 24098 Kiel, Germany.

出版信息

Proc Natl Acad Sci U S A. 2017 Jan 10;114(2):E219-E227. doi: 10.1073/pnas.1611684114. Epub 2016 Dec 27.

Abstract

The thick ascending limb (TAL) of Henle's loop drives paracellular Na, Ca, and Mg reabsorption via the tight junction (TJ). The TJ is composed of claudins that consist of four transmembrane segments, two extracellular segments (ECS1 and -2), and one intracellular loop. Claudins interact within the same (cis) and opposing (trans) plasma membranes. The claudins Cldn10b, -16, and -19 facilitate cation reabsorption in the TAL, and their absence leads to a severe disturbance of renal ion homeostasis. We combined electrophysiological measurements on microperfused mouse TAL segments with subsequent analysis of claudin expression by immunostaining and confocal microscopy. Claudin interaction properties were examined using heterologous expression in the TJ-free cell line HEK 293, live-cell imaging, and Förster/FRET. To reveal determinants of interaction properties, a set of TAL claudin protein chimeras was created and analyzed. Our main findings are that (i) TAL TJs show a mosaic expression pattern of either cldn10b or cldn3/cldn16/cldn19 in a complex; (ii) TJs dominated by cldn10b prefer Na over Mg, whereas TJs dominated by cldn16 favor Mg over Na; (iii) cldn10b does not interact with other TAL claudins, whereas cldn3 and cldn16 can interact with cldn19 to form joint strands; and (iv) further claudin segments in addition to ECS2 are crucial for trans interaction. We suggest the existence of at least two spatially distinct types of paracellular channels in TAL: a cldn10b-based channel for monovalent cations such as Na and a spatially distinct site for reabsorption of divalent cations such as Ca and Mg.

摘要

亨氏袢的厚升支(TAL)通过紧密连接(TJ)驱动细胞旁钠、钙和镁的重吸收。紧密连接由紧密连接蛋白组成,紧密连接蛋白包含四个跨膜结构域、两个细胞外结构域(ECS1和ECS2)以及一个细胞内环。紧密连接蛋白在同一(顺式)和相对(反式)质膜内相互作用。紧密连接蛋白Cldn10b、-16和-19促进TAL中的阳离子重吸收,它们的缺失会导致肾离子稳态的严重紊乱。我们将对微灌流小鼠TAL节段的电生理测量与随后通过免疫染色和共聚焦显微镜分析紧密连接蛋白的表达相结合。使用在无紧密连接的细胞系HEK 293中的异源表达、活细胞成像和Förster/荧光共振能量转移(FRET)来检测紧密连接蛋白的相互作用特性。为了揭示相互作用特性的决定因素,构建并分析了一组TAL紧密连接蛋白嵌合体。我们的主要发现是:(i)TAL紧密连接在复合物中呈现cldn10b或cldn3/cldn16/cldn19的镶嵌表达模式;(ii)以cldn10b为主的紧密连接优先重吸收钠而非镁,而以cldn16为主的紧密连接优先重吸收镁而非钠;(iii)cldn10b不与其他TAL紧密连接蛋白相互作用,而cldn3和cldn16可以与cldn19相互作用形成联合链;(iv)除了ECS2之外,其他紧密连接蛋白结构域对于反式相互作用也至关重要。我们认为TAL中至少存在两种空间上不同类型的细胞旁通道:一种基于cldn10b的单价阳离子(如钠)通道和一个空间上不同的二价阳离子(如钙和镁)重吸收位点。

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