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Structural determinants and functional consequences of protein affinity for membrane rafts

机译:蛋白质对膜筏的亲和力的结构决定因素和功能后果

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摘要

Eukaryotic plasma membranes are compartmentalized into functional lateral domains, including lipid-driven membrane rafts. Rafts are involved in most plasma membrane functions by selective recruitment and retention of specific proteins. However, the structural determinants of transmembrane protein partitioning to raft domains are not fully understood. Hypothesizing that protein transmembrane domains (TMDs) determine raft association, here we directly quantify raft affinity for dozens of TMDs. We identify three physical features that independently affect raft partitioning, namely TMD surface area, length, and palmitoylation. We rationalize these findings into a mechanistic, physical model that predicts raft affinity from the protein sequence. Application of these concepts to the human proteome reveals that plasma membrane proteins have higher raft affinity than those of intracellular membranes, consistent with raft-mediated plasma membrane sorting. Overall, our experimental observations and physical model establish general rules for raft partitioning of TMDs and support the central role of rafts in membrane traffic.
机译:真核细胞质膜被分隔成功能性的横向区域,包括脂质驱动的膜筏。筏通过选择性募集和保留特定蛋白质而参与大多数质膜功能。但是,跨膜蛋白分配到筏域的结构决定因素尚未完全了解。假设蛋白质跨膜结构域(TMDs)决定了筏的关联,在这里我们直接量化数十个TMD的筏亲和力。我们确定了三个独立影响木筏分区的物理特征,即TMD表面积,长度和棕榈酰化。我们将这些发现合理化为一种机械的物理模型,该模型可根据蛋白质序列预测筏的亲和力。这些概念在人类蛋白质组学中的应用表明,质膜蛋白比细胞内膜具有更高的筏亲和力,这与筏介导的质膜分选相一致。总体而言,我们的实验观察结果和物理模型为TMD的筏板划分建立了通用规则,并支持了筏板在膜运输中的核心作用。

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