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NCAM Ig1-2-3的结构与相互作用提示了一种新的嗜同性黏附拉链机制。

Structure and interactions of NCAM Ig1-2-3 suggest a novel zipper mechanism for homophilic adhesion.

作者信息

Soroka Vladislav, Kolkova Kateryna, Kastrup Jette S, Diederichs Kay, Breed Jason, Kiselyov Vladislav V, Poulsen Flemming M, Larsen Ingrid K, Welte Wolfram, Berezin Vladimir, Bock Elisabeth, Kasper Christina

机构信息

Protein Laboratory, Institute of Molecular Pathology, Panum Institute, Blegdamsvej 3 C, DK-2200 Copenhagen, Denmark.

出版信息

Structure. 2003 Oct;11(10):1291-301. doi: 10.1016/j.str.2003.09.006.

Abstract

The neural cell adhesion molecule, NCAM, mediates Ca(2+)-independent cell-cell and cell-substratum adhesion via homophilic (NCAM-NCAM) and heterophilic (NCAM-non-NCAM molecules) binding. NCAM plays a key role in neural development, regeneration, and synaptic plasticity, including learning and memory consolidation. The crystal structure of a fragment comprising the three N-terminal Ig modules of rat NCAM has been determined to 2.0 A resolution. Based on crystallographic data and biological experiments we present a novel model for NCAM homophilic binding. The Ig1 and Ig2 modules mediate dimerization of NCAM molecules situated on the same cell surface (cis interactions), whereas the Ig3 module mediates interactions between NCAM molecules expressed on the surface of opposing cells (trans interactions) through simultaneous binding to the Ig1 and Ig2 modules. This arrangement results in two perpendicular zippers forming a double zipper-like NCAM adhesion complex.

摘要

神经细胞黏附分子(NCAM)通过同源性(NCAM-NCAM)和异源性(NCAM-非NCAM分子)结合介导不依赖钙离子的细胞-细胞及细胞-基质黏附。NCAM在神经发育、再生以及突触可塑性(包括学习和记忆巩固)中发挥关键作用。已确定大鼠NCAM包含三个N端免疫球蛋白(Ig)模块的片段的晶体结构,分辨率为2.0埃。基于晶体学数据和生物学实验,我们提出了一种NCAM同源性结合的新模型。Ig1和Ig2模块介导位于同一细胞表面的NCAM分子的二聚化(顺式相互作用),而Ig3模块通过同时结合Ig1和Ig2模块介导位于相对细胞表面的NCAM分子之间的相互作用(反式相互作用)。这种排列导致形成两个垂直的拉链,构成类似双拉链的NCAM黏附复合体。

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