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跨膜α螺旋的二聚化基序。

A dimerization motif for transmembrane alpha-helices.

作者信息

Lemmon M A, Treutlein H R, Adams P D, Brünger A T, Engelman D M

机构信息

Department of Molecular Biophysics & Biochemistry, Yale University, New Haven, CT 06520, USA.

出版信息

Nat Struct Biol. 1994 Mar;1(3):157-63. doi: 10.1038/nsb0394-157.

Abstract

Specific helix-helix interactions inside lipid bilayers guide the folding and assembly of many integral membrane proteins and their complexes. We report here a pattern of 7 amino acids (LIxxGVxxGVxxT) which when introduced into several hydrophobic transmembrane alpha-helices promotes their specific dimerization. Dimerization is driven by interactions that are specific, dominated by the helix-helix interface, and involve no potentially ionizable groups. The motif may provide a useful tool for the functional analysis of such interactions in a variety of systems. Further, since this particular motif is rare, whilst specific helix association is not, many other such motifs may exist, which could permit sorting within complex membranes as well as guiding folding and oligomerization.

摘要

脂质双分子层内部特定的螺旋-螺旋相互作用引导着许多整合膜蛋白及其复合物的折叠和组装。我们在此报告一种由7个氨基酸组成的模式(LIxxGVxxGVxxT),当将其引入几个疏水跨膜α-螺旋时,可促进它们的特异性二聚化。二聚化由特异性相互作用驱动,这种相互作用以螺旋-螺旋界面为主导,且不涉及潜在的可电离基团。该基序可能为在各种系统中对此类相互作用进行功能分析提供有用的工具。此外,由于这种特定基序很少见,而特异性螺旋缔合并非如此,可能存在许多其他此类基序,这可以允许在复杂膜内进行分选,同时引导折叠和寡聚化。

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