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首页> 外文期刊>Journal of Biomolecular Structure and Dynamics >NS2B/NS3 protease: allosteric effect of mutations associated with the pathogenicity of tick-borne encephalitis virus.
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NS2B/NS3 protease: allosteric effect of mutations associated with the pathogenicity of tick-borne encephalitis virus.

机译:NS2B / NS3蛋白酶:与tick传脑炎病毒的致病性相关的突变的变构作用。

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摘要

The sequences of the protease domain of the tick-borne encephalitis (TBE) virus NS3 protein have two amino acid substitutions, 16 R→K and 45 S→F, in the highly pathogenic and poorly pathogenic strains of the virus, respectively. Two models of the NS2B-NS3 protease complex for the highly pathogenic and poorly pathogenic strains of the virus were constructed by homology modeling using the crystal structure of West Nile virus NS2B-NS3 protease as a template; 20?ns molecular dynamic simulations were performed for both models, the trajectories of the dynamic simulations were compared, and the averaged distance between the two models was calculated for each residue. Conformational differences between two models were revealed in the identified pocket. The different conformations of the pocket resulted in different orientations of the NS2B segment located near the catalytic triad. In the model of the highly pathogenic TBE virus the identified pocket had a more open conformation compared to the poorly pathogenic model. We propose that conformational changes in the active protease center, caused by two amino acid substitutions, can influence enzyme functioning and the virulence of the virus.
机译:tick传脑炎(TBE)脑炎病毒(NS3)蛋白的蛋白酶结构域序列在该病毒的高致病性和低致病性菌株中分别具有两个氨基酸取代,分别为16 R→K和45 S→F。以西尼罗河病毒NS2B-NS3蛋白酶的晶体结构为模板,通过同源性建模,建立了两种病毒高致病性和低致病性菌株的NS2B-NS3蛋白酶复合物模型;对两个模型进行了20?ns分子动力学模拟,比较了动力学模拟的轨迹,并针对每个残基计算了两个模型之间的平均距离。在确定的口袋中发现了两个模型之间的构象差异。口袋的不同构型导致位于催化三联体附近的NS2B节段的取向不同。在高致病性TBE病毒模型中,与致病性较差的模型相比,鉴定出的口袋具有更开放的构象。我们建议由两个氨基酸取代引起的活性蛋白酶中心的构象变化可以影响酶的功能和病毒的毒力。

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