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CRAC肽胆固醇结合功能的紊乱:一项分子动力学研究

Disorder in cholesterol-binding functionality of CRAC peptides: a molecular dynamics study.

作者信息

Miller Cayla M, Brown Angela C, Mittal Jeetain

机构信息

Department of Chemical and Biomolecular Engineering, Lehigh University , Bethlehem, Pennsylvania 18015, United States.

出版信息

J Phys Chem B. 2014 Nov 20;118(46):13169-74. doi: 10.1021/jp5106423. Epub 2014 Nov 10.

Abstract

The cholesterol recognition/interaction amino acid consensus (CRAC) motif is a primary structure pattern used to identify regions that may be responsible for preferential cholesterol binding in many proteins. The leukotoxin LtxA, which is produced by a pathogenic bacterium, contains two CRAC seqences, only one of which is responsible for cholesterol binding, and the binding is required for cytotoxicity. The factors, in addition to the CRAC definition, that may be responsible for cholesterol-binding functionality and atomistic interactions between the CRAC region and cholesterol are as yet unknown. This study uses molecular dynamics simulations to identify structural characteristics and specific interactions of the two LtxA CRAC peptides with both pure phospholipid and binary cholesterol-phospholipid bilayers. We have identified changes in the secondary structure of these peptides that occur upon cholesterol binding, which are not seen when it is associated with a cholesterol-devoid membrane, and which show salient coupling of structural disorder and function. Additionally, the central tyrosine residue of the CRAC motif was found to play a significant role in cholesterol binding, though residues outside of the CRAC motif also influence membrane interactions and functionality of the CRAC region.

摘要

胆固醇识别/相互作用氨基酸共有序列(CRAC)基序是一种一级结构模式,用于识别许多蛋白质中可能负责优先结合胆固醇的区域。由一种致病细菌产生的白细胞毒素LtxA包含两个CRAC序列,其中只有一个负责胆固醇结合,且这种结合是细胞毒性所必需的。除了CRAC定义之外,可能导致胆固醇结合功能以及CRAC区域与胆固醇之间原子相互作用的因素尚不清楚。本研究使用分子动力学模拟来识别两种LtxA CRAC肽与纯磷脂双层和胆固醇 - 磷脂二元双层的结构特征及特定相互作用。我们已经确定了这些肽在胆固醇结合时二级结构的变化,当它们与不含胆固醇的膜结合时未观察到这种变化,并且这种变化显示出结构无序与功能之间的显著耦合。此外,发现CRAC基序的中心酪氨酸残基在胆固醇结合中起重要作用,尽管CRAC基序之外的残基也会影响膜相互作用和CRAC区域的功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/44db/4242004/fc3497fc2427/jp-2014-106423_0002.jpg

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