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脂质协同作用作为 PH 结构域招募膜的一般原理。

Lipid Cooperativity as a General Membrane-Recruitment Principle for PH Domains.

机构信息

Structural and Computational Biology Unit, European Molecular Biology Laboratory (EMBL), Meyerhofstrasse 1, 69117 Heidelberg, Germany.

Structural and Computational Biology Unit, European Molecular Biology Laboratory (EMBL), Meyerhofstrasse 1, 69117 Heidelberg, Germany; Cell Biology and Biophysics Unit, EMBL, Meyerhofstrasse 1, 69117 Heidelberg, Germany.

出版信息

Cell Rep. 2015 Sep 1;12(9):1519-30. doi: 10.1016/j.celrep.2015.07.054. Epub 2015 Aug 20.

Abstract

Many cellular processes involve the recruitment of proteins to specific membranes, which are decorated with distinctive lipids that act as docking sites. The phosphoinositides form signaling hubs, and we examine mechanisms underlying recruitment. We applied a physiological, quantitative, liposome microarray-based assay to measure the membrane-binding properties of 91 pleckstrin homology (PH) domains, the most common phosphoinositide-binding target. 10,514 experiments quantified the role of phosphoinositides in membrane recruitment. For most domains examined, the observed binding specificity implied cooperativity with additional signaling lipids. Analyses of PH domains with similar lipid-binding profiles identified a conserved motif, mutations in which-including some found in human cancers-induced discrete changes in binding affinities in vitro and protein mislocalization in vivo. The data set reveals cooperativity as a key mechanism for membrane recruitment and, by enabling the interpretation of disease-associated mutations, suggests avenues for the design of small molecules targeting PH domains.

摘要

许多细胞过程涉及蛋白质被招募到特定的膜上,这些膜上装饰着独特的脂质,作为停泊位点。磷酸肌醇形成信号枢纽,我们研究了招募的机制。我们应用了一种基于生理、定量、脂质体微阵列的测定法,来测量 91 个 Pleckstrin 同源(PH)结构域的膜结合特性,这是最常见的磷酸肌醇结合靶标。10514 次实验量化了磷酸肌醇在膜招募中的作用。对于大多数检查过的结构域,观察到的结合特异性暗示了与其他信号脂质的协同作用。对具有相似脂质结合谱的 PH 结构域的分析确定了一个保守的基序,该基序中的突变,包括一些在人类癌症中发现的突变,导致体外结合亲和力和体内蛋白质定位的离散变化。该数据集揭示了协同作用是膜招募的关键机制,并通过能够解释与疾病相关的突变,为针对 PH 结构域的小分子设计提供了途径。

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