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首页> 外文期刊>Protein Science: A Publication of the Protein Society >Computational analysis of the transient movement of helices in sensory rhodopsin II.
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Computational analysis of the transient movement of helices in sensory rhodopsin II.

机译:感官视紫红质中螺旋的瞬时运动的计算分析。

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摘要

MD simulation of sensory rhodopsin II was executed for three intermediates (ground-state, K-state, M-state) appearing in its photocycle. We observed a large displacement of the cytoplasmic side of helixF only in M-state among the three intermediates. This displacement was transmitted to TM2, and the cytoplasmic side of TM2 rotated clockwise. These transient movements are in agreement with the results of an EPR experiment. That is, the early stage of signal transduction in a sRII-HtrII complex was successfully reproduced by the in silico MD simulation. By analyzing the structure of the sRII-HtrII complex, the following findings about the photocycle of sRII were obtained: (1) The hydrogen bonds between helixF and other helices determine the direction of the movement of helixF; (2) three amino acids (Arg162, Thr189, Tyr199) are essential for sRII-HtrII binding and contribute to the motion transfer from sRII to HtrII; (3) after the isomerization of retinal, a major conformational change of retinal was caused by proton transfer from Schiff base to Asp75, which, in turn, triggers the steric collision of retinal with Trp171. This is the main reason for the movement of the cytoplasmic side of helixF.
机译:对在其光周期中出现的三个中间体(基态,K态,M态)进行了视紫红质II的MD模拟。我们观察到只有在三个中间体之间处于M状态的helixF的胞质侧的大位移。该位移被传递给TM2,并且TM2的细胞质侧顺时针旋转。这些瞬时运动与EPR实验的结果一致。即,通过计算机模拟MD成功地再现了sRII-HtrII复合物中信号转导的早期阶段。通过分析sRII-HtrII配合物的结构,得到有关sRII光循环的以下发现:(1)螺旋F和其他螺旋之间的氢键决定了螺旋F的运动方向; (2)三个氨基酸(Arg162,Thr189,Tyr199)对于sRII-HtrII结合是必不可少的,并有助于从sRII到HtrII的运动转移。 (3)视网膜异构化后,视网膜的主要构象变化是由质子从席夫碱转移到Asp75引起的,进而触发了视网膜与Trp171的空间碰撞。这是helixF的细胞质侧移动的主要原因。

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