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Protein Dynamical Transition : Role of Methyl Dynamics and Local Diffusion

机译:蛋白质动态转变:甲基动力学和局部扩散的作用

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The temperature-dependent protein dynamical transition is investigated using the Instanteous Normal mode analysis (INM) and molecular dynamics (MD) simulation of crystalline myoglobin and Toxin II. The onset of anharmonic dynamics in myoglobin is observed at 150 K, far below the much-studied solvent-activated dynamical transition at 220 K. A significant fraction of methyl groups exhibit nanosecond anharmonic rotational jump diffusion at 150 K indicating the essential role of methyl dynamics in the low-temperature onset of anharmonic protein dynamics. The methyl groups that exhibit many rotational excitations are located near xenon cavities, suggesting that cavities in proteins act as activation centers of anharmonic dynamics. INM analysis of Toxin II indicates the presence of non-zero barrier-crossing, diffusive degrees of freedom accessible to the protein below the dynamical transition. The number of these diffusive degrees of freedom increases abruptly at the dynamical transition. In summary, the present investigation suggests that local diffusive processes (for example, methyl dynamics) are activated at low temperatures (much below 220 K) leading to global diffusive protein dynamics (this involves excitation of many protein atoms) at the dynamical transition.
机译:使用Instanteous正常模式分析(INM)和分子动力学结晶肌红蛋白和毒素II的(MD)模拟温度依赖性蛋白动力学过渡进行了研究。在肌红蛋白非谐动力学的发作,在150 K被观察到的,远低于在220的甲基基团K.甲显著分数备受研究溶剂活化动力学过渡在150ķ表现出纳秒非谐旋转跳扩散指示甲基动力学的重要作用在非谐蛋白动力学的低温发作。表现出许多旋转激励的甲基基团位于靠近氙空腔,这表明在蛋白质空腔充当非调谐动力学的激活中心。毒素II的INM分析表明非零屏障交叉,以动力学过渡低于蛋白质访问扩散自由度的存在。这些扩散自由度的数量在动力过渡突然增加。总之,本研究表明,局部扩散过程(例如,甲基动力学)在低温下(远低于220 K)导致全球扩散蛋白动力学(这涉及到许多蛋白质原子的激发)在动态转变激活。

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