Structural Biology on Molecular Mechanism of Low-Affinity Protein-Protein Interactions on the Cell Membrane

T. Nogi
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Abstract

Protein-protein interactions are essential in diverse cellular processes including signal transduction. It is not uncommon for protein-protein interactions in the transmembrane signaling to exhibit low binding affinities with a dissociation constant in the μM range or higher. Presumably, membrane proteins can selectively bind with their binding partners via low-affinity interactions because they can only diffuse laterally in the membrane plane and interact with the partners within a limited space on the membrane surface or within the membrane. This review focuses on the crystallographic studies on cell-surface receptors and intramembrane proteases that perform the transmembrane signaling mediated by low-affinity protein-protein interactions.
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细胞膜上低亲和蛋白相互作用分子机制的结构生物学研究
蛋白质之间的相互作用在包括信号转导在内的多种细胞过程中是必不可少的。在跨膜信号传导中,蛋白质-蛋白质相互作用表现出低结合亲和力,解离常数在μM范围内或更高,这并不罕见。据推测,膜蛋白可以通过低亲和相互作用选择性地与它们的结合伙伴结合,因为它们只能在膜平面上横向扩散,并在膜表面或膜内的有限空间内与伙伴相互作用。本文综述了低亲和蛋白-蛋白相互作用介导的跨膜信号传导的细胞表面受体和膜内蛋白酶的晶体学研究。
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