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膜蛋白的结构

Structures of membrane proteins.

作者信息

Kennedy S J

出版信息

J Membr Biol. 1978 Sep 19;42(3):265-79. doi: 10.1007/BF01870362.

Abstract

The possible conformations of integral membrane proteins are restricted by the nature of their environment. In order to satisfy the requirement of maximum hydrogen bonding, those portions of the polypeptide chain which are in contact with lipid hydrocarbon must be organized into regions of regular secondary structure. As possible models of the intramembranous regions of integral membrane proteins, three types of regular structures are discussed. Two, the alpha helix and the beta-pleated sheet, are regularly occurring structural features of soluble proteins. The third is a newly proposed class of conformations called beta helices. These helices have unique features which make them particularly well-suited to the lipid bilayer environment. The central segment of the membrane-spanning protein glycophorin can be arranged into a beta helix with a hydrophobic exterior and a polar interior containing charged amino-acid side chains. Such structures could function as transmembrane ion channels. A model of the activation process based on a hypothetical equilibrium between alpha and beta helical forms of a transmembrane protein is presented. The model can accurately reproduce the kinetics and voltage dependence of the channels in nerve.

摘要

整合膜蛋白的可能构象受到其所处环境性质的限制。为了满足最大程度氢键结合的要求,多肽链中与脂质烃接触的那些部分必须被组织成规则二级结构区域。作为整合膜蛋白膜内区域的可能模型,讨论了三种类型的规则结构。其中两种,即α螺旋和β折叠片,是可溶性蛋白质中常见的结构特征。第三种是新提出的一类构象,称为β螺旋。这些螺旋具有独特的特征,使其特别适合脂质双分子层环境。跨膜蛋白血型糖蛋白的中央片段可以排列成具有疏水外部和包含带电荷氨基酸侧链的极性内部的β螺旋。这样的结构可以作为跨膜离子通道发挥作用。提出了一个基于跨膜蛋白α螺旋和β螺旋形式之间假设平衡的激活过程模型。该模型可以准确再现神经中通道的动力学和电压依赖性。

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