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通过元动力学探索人酪蛋白激酶催化亚基的构象灵活性。

Conformational flexibility of human casein kinase catalytic subunit explored by metadynamics.

作者信息

Gouron Aurélie, Milet Anne, Jamet Helene

机构信息

DCM, Equipe Chimie Théorique, Université Joseph Fourier Grenoble-I, UMR-CNRS 5250, ICMG, FR 2607, BP 53, 38041 Grenoble Cedex 9, France.

DCM, Equipe Chimie Théorique, Université Joseph Fourier Grenoble-I, UMR-CNRS 5250, ICMG, FR 2607, BP 53, 38041 Grenoble Cedex 9, France.

出版信息

Biophys J. 2014 Mar 4;106(5):1134-41. doi: 10.1016/j.bpj.2014.01.031.

Abstract

Casein kinase CK2 is an essential enzyme in higher organisms, catalyzing the transfer of the γ phosphate from ATP to serine and threonine residues on protein substrates. In a number of animal tumors, CK2 activity has been shown to escape normal cellular control, making it a potential target for cancer therapy. Several crystal structures of human CK2 have been published with different conformations for the CK2α catalytic subunit. This variability reflects a high flexibility for two regions of CK2α: the interdomain hinge region, and the glycine-rich loop (p-loop). Here, we present a computational study simulating the equilibrium between three conformations involving these regions. Simulations were performed using well-tempered metadynamics combined with a path collective variables approach. This provides a reference pathway describing the conformational changes being studied, based on analysis of free energy surfaces. The free energies of the three conformations were found to be close and the paths proposed had low activation barriers. Our results indicate that these conformations can exist in water. This information should be useful when designing inhibitors specific to one conformation.

摘要

酪蛋白激酶CK2是高等生物中的一种必需酶,催化将ATP中的γ磷酸基团转移到蛋白质底物上的丝氨酸和苏氨酸残基上。在许多动物肿瘤中,已表明CK2活性不受正常细胞控制,使其成为癌症治疗的潜在靶点。已发表了几种人CK2的晶体结构,其中CK2α催化亚基具有不同的构象。这种变异性反映了CK2α两个区域的高度灵活性:结构域间铰链区和富含甘氨酸的环(p环)。在这里,我们进行了一项计算研究,模拟涉及这些区域的三种构象之间的平衡。使用温和的元动力学结合路径集体变量方法进行模拟。基于自由能表面分析,这提供了一条描述正在研究的构象变化的参考路径。发现三种构象的自由能接近,并且提出的路径具有较低的活化能垒。我们的结果表明这些构象可以在水中存在。在设计针对一种构象的抑制剂时,这些信息应该是有用的。

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