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Anatomy and Dynamics of a Supramolecular Membrane Protein Cluster

机译:超分子膜蛋白簇的解剖与动力学

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Most plasmalemmal proteins organize in submicrometer-sized clusters whose architecture and dynamics are still enigmatic. With syntaxin 1 as an example, we applied a combination of far-field optical nanoscopy, biochemistry, fluorescence recovery after photobleaching (FRAP) analysis, and simulations to show that clustering can be explained by self-organization based on simple physical principles. On average, the syntaxin clusters exhibit a diameter of 50 to 60 nanometers and contain 75 densely crowded syntaxins that dynamically exchange with freely diffusing molecules. Self-association depends on weak homophilk protein-protein interactions. Simulations suggest that clustering immobilizes and conformationally constrains the molecules. Moreover, a balance between self-association and crowdinginduced steric repulsions is sufficient to explain both the size and dynamics of syntaxin clusters and likely of many oligomerizing membrane proteins that form supramolecular structures.
机译:大多数血浆中的蛋白质组织在亚微米大小的簇中,其结构和动力学仍然难以捉摸。以syntaxin 1为例,我们结合了远场光学纳米技术,生物化学,光漂白后的荧光恢复(FRAP)分析和模拟,以证明可以通过基于简单物理原理的自组织来解释聚类。平均而言,语法素簇的直径为50至60纳米,并包含75个密集拥挤的语法素,可与自由扩散的分子动态交换。自我关联取决于弱的同质蛋白之间的相互作用。模拟表明,聚簇固定并构象约束了分子。此外,自我联系和拥挤诱导的空间排斥之间的平衡足以解释语法句法簇的大小和动力学,以及可能解释形成超分子结构的许多低聚膜蛋白的大小和动力学。

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