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膜蛋白结构中的脂质。

Lipids in membrane protein structures.

作者信息

Palsdottir Hildur, Hunte Carola

机构信息

Department of Molecular Membrane Biology, Max-Planck-Institute of Biophysics, Marie-Curie-Strasse 15, D-60439 Frankfurt, Germany.

出版信息

Biochim Biophys Acta. 2004 Nov 3;1666(1-2):2-18. doi: 10.1016/j.bbamem.2004.06.012.

Abstract

This review describes the recent knowledge about tightly bound lipids in membrane protein structures and deduces general principles of the binding interactions. Bound lipids are grouped in annular, nonannular, and integral protein lipids. The importance of lipid binding for vertical positioning and tight integration of proteins in the membrane, for assembly and stabilization of oligomeric and multisubunit complexes, for supercomplexes, as well as their functional roles are pointed out. Lipid binding is stabilized by multiple noncovalent interactions from protein residues to lipid head groups and hydrophobic tails. Based on analysis of lipids with refined head groups in membrane protein structures, distinct motifs were identified for stabilizing interactions between the phosphodiester moieties and side chains of amino acid residues. Differences between binding at the electropositive and electronegative membrane side, as well as a preferential binding to the latter, are observed. A first attempt to identify lipid head group specific binding motifs is made. A newly identified cardiolipin binding site in the yeast cytochrome bc(1) complex is described. Assignment of unsaturated lipid chains and evolutionary aspects of lipid binding are discussed.

摘要

本综述描述了关于膜蛋白结构中紧密结合脂质的最新知识,并推导了结合相互作用的一般原理。结合的脂质分为环形、非环形和整合蛋白脂质。指出了脂质结合对于蛋白质在膜中的垂直定位和紧密整合、对于寡聚体和多亚基复合物的组装和稳定、对于超复合物的重要性及其功能作用。脂质结合通过从蛋白质残基到脂质头部基团和疏水尾部的多种非共价相互作用得以稳定。基于对膜蛋白结构中具有精细头部基团的脂质的分析,鉴定出了用于稳定磷酸二酯部分与氨基酸残基侧链之间相互作用的不同基序。观察到在膜的正电侧和负电侧结合的差异,以及对后者的优先结合。首次尝试鉴定脂质头部基团特异性结合基序。描述了在酵母细胞色素bc(1)复合物中新鉴定的心磷脂结合位点。讨论了不饱和脂质链的分配和脂质结合的进化方面。

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