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CIPP是一种新型多价PDZ结构域蛋白,可选择性地与Kir4.0家族成员、NMDA受体亚基、神经连接蛋白和神经配蛋白相互作用。

CIPP, a novel multivalent PDZ domain protein, selectively interacts with Kir4.0 family members, NMDA receptor subunits, neurexins, and neuroligins.

作者信息

Kurschner C, Mermelstein P G, Holden W T, Surmeier D J

机构信息

Department of Developmental Neurobiology, Saint Jude Children's Research Hospital, Memphis, Tennessee, 38105, USA.

出版信息

Mol Cell Neurosci. 1998 Jun;11(3):161-72. doi: 10.1006/mcne.1998.0679.

Abstract

We report a novel multivalent PDZ domain protein, CIPP (for channel-interacting PDZ domain protein), which is expressed exclusively in brain and kidney. Within the brain, the highest CIPP mRNA levels were found in neurons of the cerebellum, inferior colliculus, vestibular nucleus, facial nucleus, and thalamus. Furthermore, we identified the inward rectifier K+ (Kir) channel, Kir4.1 (also called "Kir1.2"), as a cellular CIPP ligand. Among several other Kir channels tested, only the closely related Kir4.2 (or "Kir1.3") also interacted with CIPP. In addition, specific PDZ domains within CIPP associated selectively with the C-termini of N-methyl-D-aspartate subtypes of glutamate receptors, as well as neurexins and neuroligins, cell surface molecules enriched in synaptic membranes. Thus, CIPP may serve as a scaffold that brings structurally diverse but functionally connected proteins into close proximity at the synapse. The functional consequences of CIPP expression on Kir4.1 channels were studied using whole-cell voltage clamp techniques in Kir4.1 transfected COS-7 cells. On average, Kir4.1 current densities were doubled by cotransfection with CIPP.

摘要

我们报道了一种新型多价PDZ结构域蛋白CIPP(通道相互作用PDZ结构域蛋白),它仅在脑和肾中表达。在脑中,小脑、下丘、前庭核、面神经核和丘脑的神经元中CIPP mRNA水平最高。此外,我们鉴定出内向整流钾离子(Kir)通道Kir4.1(也称为“Kir1.2”)是细胞内CIPP的配体。在测试的其他几种Kir通道中,只有密切相关的Kir4.2(或“Kir1.3”)也与CIPP相互作用。此外,CIPP内的特定PDZ结构域选择性地与谷氨酸受体N-甲基-D-天冬氨酸亚型的C末端以及富集于突触膜的细胞表面分子神经连接蛋白和神经配体相关联。因此,CIPP可能作为一种支架,使结构多样但功能相关的蛋白质在突触处紧密靠近。利用全细胞膜片钳技术在转染Kir4.1的COS-7细胞中研究了CIPP表达对Kir4.1通道的功能影响。平均而言,与CIPP共转染使Kir4.1电流密度增加了一倍。

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