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Conformational dynamics of a G-protein α subunit is tightly regulated by nucleotide binding

机译:G蛋白α亚基的构象动力学受核苷酸结合的严格调控

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摘要

Heterotrimeric G proteins play a pivotal role in the signal-transduction pathways initiated by G-protein-coupled receptor (GPCR) activation. Agonist-receptor binding causes GDP-to-GTP exchange and dissociation of the Gα subunit from the heterotrimeric G protein, leading to downstream signaling. Here, we studied the internal mobility of a G-protein α subunit in its apo and nucleotide-bound forms and characterized their dynamical features at multiple time scales using solution NMR, small-angle X-ray scattering, and molecular dynamics simulations. We find that binding of GTP analogs leads to a rigid and closed arrangement of the Gα subdomain, whereas the apo and GDP-bound forms are considerably more open and dynamic. Furthermore, we were able to detect two conformational states of the Gα Ras domain in slow exchange whose populations are regulated by binding to nucleotides and a GPCR. One of these conformational states, the open state, binds to the GPCR; the second conformation, the closed state, shows no interaction with the receptor. Binding to the GPCR stabilizes the open state. This study provides an in-depth analysis of the conformational landscape and the switching function of a G-protein α subunit and the influence of a GPCR in that landscape.
机译:异三聚体G蛋白在G蛋白偶联受体(GPCR)激活引发的信号转导途径中起着关键作用。激动剂-受体结合引起GDP-GTP交换和Gα亚基与异三聚体G蛋白的解离,从而导致下游信号传导。在这里,我们研究了G蛋白α亚基的载脂蛋白和核苷酸结合形式的内部迁移率,并使用溶液NMR,小角度X射线散射和分子动力学模拟在多个时间尺度上表征了它们的动力学特征。我们发现,GTP类似物的结合导致Gα子域的刚性和封闭排列,而载脂蛋白和GDP结合形式则更为开放和动态。此外,我们能够在慢速交换中检测GαRas结构域的两个构象状态,其种群受核苷酸结合和GPCR的调控。这些构象状态之一,即开放状态,与GPCR结合;第二种构型,即闭合状态,表明与受体没有相互作用。与GPCR的结合可稳定开放状态。这项研究提供了深入的构象格局和G蛋白α亚基的转换功能以及GPCR在该格局中的影响的分析。

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