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间隙连接通道的分子建模与诱变

Molecular modeling and mutagenesis of gap junction channels.

作者信息

Kovacs Julio A, Baker Kent A, Altenberg Guillermo A, Abagyan Ruben, Yeager Mark

机构信息

Department of Molecular Biology, The Scripps Research Institute, La Jolla, CA 92037, USA.

出版信息

Prog Biophys Mol Biol. 2007 May-Jun;94(1-2):15-28. doi: 10.1016/j.pbiomolbio.2007.03.013. Epub 2007 Mar 23.

Abstract

Gap junction channels connect the cytoplasms of adjacent cells through the end-to-end docking of hexameric hemichannels called connexons. Each connexon is formed by a ring of 24 alpha-helices that are staggered by 30 degrees with respect to those in the apposed connexon. Current evidence suggests that the two connexons are docked by interdigitated, anti-parallel beta strands across the extracellular gap. The second extracellular loop, E2, guides selectivity in docking between connexons formed by different isoforms. There is considerably more sequence variability of the N-terminal portion of E2, suggesting that this region dictates connexon coupling. Mutagenesis, biochemical, dye-transfer and electrophysiological data, combined with computational studies, have suggested possible assignments for the four transmembrane alpha-helices within each subunit. Most current models assign M3 as the major pore-lining helix. Mapping of human mutations onto a C(alpha) model suggested that native helix packing is important for the formation of fully functional channels. Nevertheless, a mutant in which the M4 helix has been replaced with polyalanine is functional, suggesting that M4 is located on the perimeter of the channel. In spite of this substantial progress in understanding the structural biology of gap junction channels, an experimentally determined structure at atomic resolution will be essential to confirm these concepts.

摘要

间隙连接通道通过称为连接子的六聚体半通道的端对端对接连接相邻细胞的细胞质。每个连接子由24个α螺旋组成的环形成,这些α螺旋相对于相对的连接子中的α螺旋错开30度。目前的证据表明,两个连接子通过跨细胞外间隙的相互交错的反平行β链对接。第二个细胞外环E2在由不同同工型形成的连接子之间的对接中引导选择性。E2的N端部分的序列变异性要大得多,这表明该区域决定连接子的偶联。诱变、生化、染料转移和电生理数据,结合计算研究,已经为每个亚基内的四个跨膜α螺旋提出了可能的归属。目前大多数模型将M3指定为主要的孔内衬螺旋。将人类突变映射到Cα模型上表明,天然螺旋堆积对于形成功能完全的通道很重要。然而,一个M4螺旋被聚丙氨酸取代的突变体是有功能的,这表明M4位于通道的周边。尽管在理解间隙连接通道的结构生物学方面取得了这一重大进展,但实验确定的原子分辨率结构对于证实这些概念至关重要。

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