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首页> 外文期刊>Scientific reports. >Mapping the Dynamic Functions and Structural Features of AcrB Efflux Pump Transporter Using Accelerated Molecular Dynamics Simulations
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Mapping the Dynamic Functions and Structural Features of AcrB Efflux Pump Transporter Using Accelerated Molecular Dynamics Simulations

机译:使用加速的分子动力学模拟绘制AcrB外排泵转运蛋白的动力学功能和结构特征

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Multidrug efflux pumps confer resistance to their bacterial hosts by pumping out a diverse range of compounds, including most antibiotics. Being more familiar with the details of functional dynamics and conformations of these types of pumps could help in discovering approaches to stop them functioning properly. Computational approaches, particularly conventional molecular dynamics simulations followed by diverse post simulation analysis, are powerful methods that help researchers by opening a new window to study phenomena that are not detectable in as much detail in vitro or in vivo as they are in silico. In this study, accelerated molecular dynamics simulations were applied to study the dynamics of AcrB efflux pump transporters in interaction with PAβN and tetracycline as an inhibitor and a substrate, respectively, to compare the differences in the dynamics and consequently the mechanism of action of the pump. The different dynamics for PAβN -bound form of AcrB compared to the TET-bound form is likely to affect the rotating mechanism typically observed for AcrB transporter. This shows the dynamics of the active AcrB transporter is different in a substrate-bound state compared to an inhibitor-bound state. This advances our knowledge and helps to unravel the mechanism of tripartite efflux pumps.
机译:多药外排泵通过抽出包括大多数抗生素在内的各种化合物,赋予其细菌宿主抗药性。更加熟悉这些类型的泵的功能动力学和构造细节,可以帮助您找到阻止其正常运行的方法。计算方法,特别是常规的分子动力学模拟以及随后的各种后期模拟分析,是一种功能强大的方法,可以通过打开一个新的窗口来研究在体外或体内无法像在计算机上一样详细地检测到的现象,从而帮助研究人员。在这项研究中,加速分子动力学模拟被用来研究AcrB外排泵转运蛋白与PAβN和四环素作为抑制剂和底物相互作用的动力学,以比较动力学的差异,从而比较泵的作用机理。 。与TET结合形式相比,AcrB的PAβN结合形式的动力学变化可能会影响AcrB转运蛋白通常观察到的旋转机制。这表明活性AcrB转运蛋白的动力学在底物结合状态与抑制剂结合状态是不同的。这提高了我们的知识,并有助于阐明三方外排泵的机理。

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