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Interplay between the folding mechanism and binding modes in folding coupled to binding processes

机译:折叠机构与折叠粘合模式之间的相互作用耦合到绑定过程

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摘要

Proteins that fold upon binding to their partners exhibit complex binding behavior such as induced-fit. But the connections between the folding mechanism and the binding mode remain unknown. Here we focus on the high affinity complex between the physiologically and marginally unstable, fast folder PSBD and the E1 subunit of pyruvate dehydrogenase. Using coarse-grained simulations we investigate the binding to E1 of a partially disordered PSBD under two folding scenarios: two-state and downhill. Our simulations show that induced-fit binding requires that PSBD folds-unfolds in the downhill folding regime. In contrast, a two-state folding PSBD must fold completely before it binds. The reason is that effective coupling between folding and binding involves partially folded conformations, which are only sufficiently populated under the downhill folding regime. Our results establish a direct mechanistic link between complex binding and downhill folding, supporting the idea that PSBD operates functionally as a conformational rheostat.
机译:在与其合作伙伴结合后折叠的蛋白质表现出诸如诱​​导的复合物的结合行为。但折叠机构和绑定模式之间的连接仍然未知。在这里,我们专注于生理学和边际不稳定,快速夹PSBD和丙酮酸脱氢酶的E1亚基之间的高亲和力复合物。使用粗粒模拟我们在两种折叠方案下调查与部分无序的PSBD的e1的结合:双态和下坡。我们的模拟表明,诱导拟合绑定要求在下坡折叠方案中展开PSBD折叠。相比之下,两个状态折叠PSBD必须在绑定之前完全折叠。原因是折叠和装订之间的有效耦合涉及部分折叠的构象,其仅在下坡折叠状态下充分填充。我们的结果建立了复杂绑定和下坡折叠之间的直接机械联系,支持PSBD在功能上运行的想法作为构象变阻器。

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