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Nucleotide Dependent Switching in Rho GTPase: Conformational Heterogeneity and Competing Molecular Interactions

机译:rho GTP酶中的核苷酸依赖性切换:构象异质性和竞争分子相互作用

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Ras superfamily of GTPases regulate myriad cellular processes through a conserved nucleotide (GTP/GDP) dependent switching mechanism. Unlike Ras family of GTPases, for the Rho GTPases, there is no clear evidence for the existence of “sub-states” such as state 1 & state 2 in the GTP bound form. To explore the nucleotide dependent conformational space of the Switch I loop and also to look for existence of state 1 like conformations in Rho GTPases, atomistic molecular dynamics and metadynamics simulations on RhoA were performed. These studies demonstrate that both the nucleotide-free state and the GDP bound “OFF” state have very similar conformations, whereas the GTP bound “ON” state has unique conformations with signatures of two intermediate states. The conformational free energy landscape for these systems suggests the presence of multiple intermediate states. Interestingly, the energetic penalty of exposing the non-polar residues in the GTP bound form is counter balanced by the favourable hydrogen bonded interactions between the γ-phosphate group of GTP with the highly conserved Tyr34 and Thr37 residues. These competing molecular interactions lead to a tuneable energy landscape of the Switch I conformation, which can undergo significant changes based on the local environment including changes upon binding to effectors.
机译:GTPases的Ras Superfamily通过保守的核苷酸(GTP / GDP)依赖性开关机构调节多种细胞过程。与RAS家族的GTP酶,对于RHO GTP酶,没有明确的证据证明在GTP绑定形式中的“子状态”如国家1和状态2。为了探讨开关I环的核苷酸依赖性构象空间,并且还寻找存在于Rho GTP酶的构象的状态1,进行原子分子动力学和RHOA的元动态模拟。这些研究表明,无核苷酸的状态和GDP结合“OFF”状态具有非常相似的构象,而GTP结合“ON”状态具有与两个中间状态的签名的独特构象。这些系统的构象自由能景观表明存在多个中间状态。有趣的是,暴露于GTP结合形式中的非极性残基的能量惩罚是通过GTP的γ-磷酸基团与高度保守的Tyr34和Thr37残基之间的有利氢键相互作用进行计数。这些竞争的分子相互作用导致开关I构象的可调能量景观,这可以基于当地环境进行显着变化,包括与效果结合时的变化。

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