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Dynamic regulation of lipid-protein interactions

机译:脂蛋白相互作用的动态调节

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We review the importance of helix motions for the function of several important categories of membrane proteins and for the properties of several model molecular systems. For voltage-gated potassium or sodium channels, sliding, tilting and/or rotational movements of the S4 helix accompanied by a swapping of cognate side-chain ion-pair interactions regulate the channel gating. In the seven-helix G protein-coupled receptors, exemplified by the rhodopsins, collective helix motions serve to activate the functional signaling. Peptides which initially associate with lipid-bilayer membrane surfaces may undergo dynamic transitions from surface-bound to tilted-transmembrane orientations, sometimes accompanied by changes in the molecularity, formation of a pore or, more generally, the activation of biological function. For single-span membrane proteins, such as the tyrosine kinases, an interplay between juxtamembrane and transmembrane domains is likely to be crucial for the regulation of dimer assembly that in turn is associated with the functional responses to external signals. Additionally, we note that experiments with designed single-span transmembrane helices offer fundamental insights into the molecular features that govern protein-lipid interactions. (C) 2015 Elsevier B.V. All rights reserved.
机译:我们审查了螺旋运动对于膜蛋白的几个重要类别的功能和几个模型分子系统的性质的重要性。对于电压门控的钾或钠通道,S4螺旋的滑动,倾斜和/或旋转运动伴随同源侧链离子对相互作用的交换,调节了通道门控。在视紫红质为例的七螺旋G蛋白偶联受体中,集体螺旋运动用于激活功能性信号传导。最初与脂质双分子层膜表面缔合的肽可能经历从表面结合到倾斜跨膜取向的动态转变,有时伴随着分子的变化,孔的形成或更一般地生物学功能的激活。对于单跨膜蛋白,例如酪氨酸激酶,近膜结构域和跨膜结构域之间的相互作用可能对调节二聚体装配至关重要,而二聚体装配又与对外部信号的功能响应相关。此外,我们注意到使用设计的单跨度跨膜螺旋进行的实验为控制蛋白质-脂质相互作用的分子特征提供了基本见识。 (C)2015 Elsevier B.V.保留所有权利。

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