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本文引用的文献

1
Identification of dynamical correlations within the myosin motor domain by the normal mode analysis of an elastic network model.通过弹性网络模型的正常模式分析鉴定肌球蛋白运动结构域内的动力学相关性。
J Mol Biol. 2005 Feb 25;346(3):745-59. doi: 10.1016/j.jmb.2004.12.020. Epub 2005 Jan 5.
2
Myosin flexibility: structural domains and collective vibrations.肌球蛋白的柔韧性:结构域与集体振动
Proteins. 2004 Feb 15;54(3):384-93. doi: 10.1002/prot.10476.
3
Analysis of functional motions in Brownian molecular machines with an efficient block normal mode approach: myosin-II and Ca2+ -ATPase.用高效块正规模式方法分析布朗分子机器中的功能运动:肌球蛋白-II和Ca2+ -ATP酶
Biophys J. 2004 Feb;86(2):743-63. doi: 10.1016/S0006-3495(04)74152-1.
4
A comparative study of motor-protein motions by using a simple elastic-network model.利用简单弹性网络模型对运动蛋白运动进行的比较研究。
Proc Natl Acad Sci U S A. 2003 Nov 11;100(23):13253-8. doi: 10.1073/pnas.2235686100. Epub 2003 Oct 29.
5
Electron cryo-microscopy shows how strong binding of myosin to actin releases nucleotide.电子冷冻显微镜显示了肌球蛋白与肌动蛋白的强结合如何释放核苷酸。
Nature. 2003 Sep 25;425(6956):423-7. doi: 10.1038/nature02005.
6
A structural state of the myosin V motor without bound nucleotide.肌球蛋白V马达无结合核苷酸时的结构状态。
Nature. 2003 Sep 25;425(6956):419-23. doi: 10.1038/nature01927.
7
A structural model for actin-induced nucleotide release in myosin.肌球蛋白中肌动蛋白诱导核苷酸释放的结构模型。
Nat Struct Biol. 2003 Oct;10(10):826-30. doi: 10.1038/nsb987. Epub 2003 Sep 21.
8
Closing of the nucleotide pocket of kinesin-family motors upon binding to microtubules.驱动蛋白家族马达蛋白与微管结合后核苷酸口袋的关闭。
Science. 2003 May 2;300(5620):798-801. doi: 10.1126/science.1082374.
9
Simplified normal mode analysis of conformational transitions in DNA-dependent polymerases: the elastic network model.DNA 依赖性聚合酶构象转变的简化正常模式分析:弹性网络模型
J Mol Biol. 2002 Jul 26;320(5):1011-24. doi: 10.1016/s0022-2836(02)00562-4.
10
Kinesin: switch I & II and the motor mechanism.驱动蛋白:开关I和II与运动机制
J Cell Sci. 2002 Jan 1;115(Pt 1):15-23. doi: 10.1242/jcs.115.1.15.

探究与全局动力学相关的核苷酸结合口袋的局部动力学:肌球蛋白与驱动蛋白。

Probing the local dynamics of nucleotide-binding pocket coupled to the global dynamics: myosin versus kinesin.

作者信息

Zheng Wenjun, Brooks Bernard R

机构信息

Laboratory of Computational Biology, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, Maryland, USA.

出版信息

Biophys J. 2005 Jul;89(1):167-78. doi: 10.1529/biophysj.105.063305. Epub 2005 May 6.

DOI:10.1529/biophysj.105.063305
PMID:15879477
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1366515/
Abstract

Based on the elastic network model, we develop a new analysis for protein complexes, which probes the local dynamics of a subsystem that is elastically coupled to a fluctuating environment. This method is applied to a comparative dynamical analysis of the nucleotide-binding pocket of two motor proteins-myosins and kinesins. In myosins, the observed structural changes in the nucleotide-pocket from the transition state to the rigorlike state are dominated by the lowest normal mode that involves significant movements in both switch I and switch II; in kinesins, the measured conformational changes in the nucleotide-pocket are also dominated by the lowest mode, which, however, only involves large movement in switch I. We then compute the global structural changes induced by the nucleotide-pocket deformations as described by the dominant pocket-mode, which yield encouraging results: in myosins, multiple hinge motions involving the opening/closing of the cleft between the upper and lower 50 -kDa subdomains and the swinging movement of the converter are induced, which are dominated by precisely the same global mode that has been recently identified by us as important to the dynamical correlations among the nucleotide-pocket, the actin-binding site, and the converter; in kinesins, the induced global conformational changes are well described by a highly collective global mode which hints for a dynamical pathway spanning from the nucleotide-pocket to the neck-linker via the H6 helix.

摘要

基于弹性网络模型,我们开发了一种针对蛋白质复合物的新分析方法,该方法探究了与波动环境弹性耦合的子系统的局部动力学。此方法应用于两种马达蛋白——肌球蛋白和驱动蛋白的核苷酸结合口袋的比较动力学分析。在肌球蛋白中,从过渡态到类似僵直态时核苷酸口袋中观察到的结构变化主要由最低简正模式主导,该模式在开关I和开关II中均涉及显著运动;在驱动蛋白中,核苷酸口袋中测量到的构象变化同样由最低模式主导,然而,该模式仅在开关I中涉及大的运动。然后,我们计算了由占主导的口袋模式所描述的核苷酸口袋变形引起的全局结构变化,结果令人鼓舞:在肌球蛋白中,诱导了多个铰链运动,包括上下50 kDa子域之间裂隙的打开/关闭以及转换器的摆动运动,这些运动恰好由我们最近确定的对核苷酸口袋、肌动蛋白结合位点和转换器之间的动力学关联很重要的相同全局模式主导;在驱动蛋白中,诱导的全局构象变化由一种高度集体的全局模式很好地描述,这暗示了一条从核苷酸口袋经H6螺旋到颈链的动力学途径。