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G13 突变诱导 GDP/K-Ras 中开关结构域构象转变的研究:通过高斯加速分子动力学模拟和主成分分析。

Conformational transformation of switch domains in GDP/K-Ras induced by G13 mutants: An investigation through Gaussian accelerated molecular dynamics simulations and principal component analysis.

机构信息

School of Science, Shandong Jiaotong University, Jinan, 250357, China.

School of Science, Shandong Jiaotong University, Jinan, 250357, China.

出版信息

Comput Biol Med. 2021 Aug;135:104639. doi: 10.1016/j.compbiomed.2021.104639. Epub 2021 Jul 7.

DOI:10.1016/j.compbiomed.2021.104639
PMID:34247129
Abstract

Mutations in K-Ras are involved in a large number of all human cancers, thus, K-Ras is regarded as a promising target for anticancer drug design. Understanding the target roles of K-Ras is important for providing insights on the molecular mechanism underlying the conformational transformation of the switch domains in K-Ras due to mutations. In this study, multiple replica Gaussian accelerated molecular (MR-GaMD) simulations and principal component analysis (PCA) were applied to probe the effect of G13A, G13D and G13I mutations on conformational transformations of the switch domains in GDP-associated K-Ras. The results suggest that G13A, G13D and G13I enhance the structural flexibility of the switch domains, change the correlated motion modes of the switch domains and strengthen the total motion strength of K-Ras compared with the wild-type (WT) K-Ras. Free energy landscape analyses not only show that the switch domains of the GDP-bound inactive K-Ras mainly exist as a closed state but also indicate that mutations evidently alter the free energy profile of K-Ras and affect the conformational transformation of the switch domains between the closed and open states. Analyses of hydrophobic interaction contacts and hydrogen bonding interactions show that the mutations scarcely change the interaction network of GDP with K-Ras and only disturb the interaction of GDP with the switch (SW1). In summary, two newly introduced mutations, G13A and G13I, play similar adjustment roles in the conformational transformations of two switch domains to G13D and are possibly utilized to tune the activity of K-Ras and the binding of guanine nucleotide exchange factors.

摘要

K-Ras 中的突变涉及到大量的人类癌症,因此,K-Ras 被认为是抗癌药物设计的一个有前途的靶点。了解 K-Ras 的靶点作用对于提供有关突变导致 K-Ras 开关结构域构象转变的分子机制的见解很重要。在这项研究中,我们应用了多个复制高斯加速分子(MR-GaMD)模拟和主成分分析(PCA)来研究 G13A、G13D 和 G13I 突变对 GDP 结合的 K-Ras 中开关结构域构象转变的影响。结果表明,与野生型(WT)K-Ras 相比,G13A、G13D 和 G13I 增强了开关结构域的结构灵活性,改变了开关结构域的相关运动模式,并增强了 K-Ras 的总运动强度。自由能景观分析不仅表明 GDP 结合的失活 K-Ras 的开关结构域主要以封闭状态存在,而且表明突变明显改变了 K-Ras 的自由能分布,并影响了开关结构域在封闭和开放状态之间的构象转变。疏水相互作用接触和氢键相互作用的分析表明,突变几乎不改变 GDP 与 K-Ras 的相互作用网络,而只是干扰 GDP 与开关(SW1)的相互作用。总之,两种新引入的突变,G13A 和 G13I,在两个开关结构域的构象转变中对 G13D 起着类似的调节作用,可能被用来调节 K-Ras 的活性和鸟嘌呤核苷酸交换因子的结合。

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