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多囊蛋白-2(TRPP2)的多聚体结构:与TRPC1形成的同型和异型多聚体的结构-功能相关性

The multimeric structure of polycystin-2 (TRPP2): structural-functional correlates of homo- and hetero-multimers with TRPC1.

作者信息

Zhang Peng, Luo Ying, Chasan Bernard, González-Perrett Silvia, Montalbetti Nicolás, Timpanaro Gustavo A, Cantero María del Rocío, Ramos Arnolt J, Goldmann Wolfgang H, Zhou Jing, Cantiello Horacio F

机构信息

Nephrology Division and Electrophysiology Core, Massachusetts General Hospital East, Charlestown, MA 02129, USA.

出版信息

Hum Mol Genet. 2009 Apr 1;18(7):1238-51. doi: 10.1093/hmg/ddp024. Epub 2009 Feb 3.

Abstract

Polycystin-2 (PC2, TRPP2), the gene product of PKD2, whose mutations cause autosomal dominant polycystic kidney disease (ADPKD), belongs to the superfamily of TRP channels. PC2 is a non-selective cation channel, with multiple subconductance states. In this report, we explored structural and functional properties of PC2 and whether the conductance substates represent monomeric contributions to the channel complex. A kinetic analysis of spontaneous channel currents of PC2 showed that four intrinsic, non-stochastic subconductance states, which followed a staircase behavior, were both pH- and voltage-dependent. To confirm the oligomeric contributions to PC2 channel function, heteromeric PC2/TRPC1 channel complexes were also functionally assessed by single channel current analysis. Low pH inhibited the PC2 currents in PC2 homomeric complexes, but failed to affect PC2 currents in PC2/TRPC1 heteromeric complexes. Amiloride, in contrast, abolished PC2 currents in both the homomeric PC2 complexes and the heteromeric PC2/TRPC1 complexes, thus PC2/TRPC1 complexes have distinct functional properties from the homomeric complexes. The topological features of the homomeric PC2-, TRPC1- and heteromeric PC2/TRPC1 channel complexes, assessed by atomic force microscopy, were consistent with structural tetramers. TRPC1 homomeric channels had different average diameter and protruding height when compared with the PC2 homomers. The contribution of individual monomers to the PC2/TRPC1 hetero-complexes was easily distinguishable. The data support tetrameric models of both the PC2 and TRPC1 channels, where the overall conductance of a particular channel will depend on the contribution of the various functional monomers in the complex.

摘要

多囊蛋白-2(PC2,TRPP2)是PKD2的基因产物,其突变会导致常染色体显性多囊肾病(ADPKD),属于瞬时受体电位(TRP)通道超家族。PC2是一种非选择性阳离子通道,具有多种亚电导状态。在本报告中,我们探究了PC2的结构和功能特性,以及这些电导亚状态是否代表通道复合体中的单体贡献。对PC2自发通道电流的动力学分析表明,四个内在的、非随机的亚电导状态呈阶梯状变化,且依赖于pH值和电压。为了确认对PC2通道功能的寡聚体贡献,还通过单通道电流分析对异源PC2/TRPC1通道复合体进行了功能评估。低pH抑制了PC2同源复合体中的PC2电流,但未能影响PC2/TRPC1异源复合体中的PC2电流。相比之下,氨氯地平消除了同源PC2复合体和异源PC2/TRPC1复合体中的PC2电流,因此PC2/TRPC1复合体具有与同源复合体不同的功能特性。通过原子力显微镜评估的同源PC2、TRPC1和异源PC2/TRPC1通道复合体的拓扑特征与结构四聚体一致。与PC2同源物相比,TRPC1同源通道具有不同的平均直径和突出高度。单个单体对PC2/TRPC1异源复合体的贡献很容易区分。这些数据支持PC2和TRPC1通道的四聚体模型,其中特定通道的总电导率将取决于复合体中各种功能单体的贡献。

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