Coarse-grained simulations of conformational changes in the multidrug efflux transporter AcrB†

IF 3.743 Q2 Biochemistry, Genetics and Molecular Biology Molecular BioSystems Pub Date : 2017-07-17 DOI:10.1039/C7MB00276A
Yead Jewel, Jin Liu and Prashanta Dutta
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引用次数: 10

Abstract

The multidrug resistance (MDR) system actively pumps antibiotics out of cells causing serious health problems. During the pumping, AcrB (one of the key components of MDR) undergoes a series of large-scale and proton-motive conformational changes. Capturing the conformational changes through all-atom simulations is challenging. Here, we implement a hybrid coarse-grained force field to investigate the conformational changes of AcrB in the porter domain under different protonation states of Asp407/Asp408 in the trans-membrane domain. Our results show that protonation of Asp408 in monomer III (extrusion) stabilizes the asymmetric structure of AcrB; deprotonation of Asp408 induces clear opening of the entrance and closing of the exit leading to the transition from extrusion to access state. The structural changes in the porter domain of AcrB are strongly coupled with the proton translocation stoichiometry in the trans-membrane domain. Moreover, our simulations support the postulation that AcrB should adopt the symmetric resting state in a substrate-free situation.

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多药外排转运体AcrB +构象变化的粗粒度模拟
多药耐药(MDR)系统主动将抗生素排出细胞,造成严重的健康问题。在抽运过程中,AcrB (MDR的关键成分之一)发生了一系列大规模的质子驱动构象变化。通过全原子模拟来捕捉构象变化是具有挑战性的。本文采用混合粗粒度力场研究了Asp407/Asp408在跨膜结构域中不同质子化状态下,转运结构域中AcrB的构象变化。结果表明,Asp408在单体III中的质子化(挤压)稳定了AcrB的不对称结构;Asp408的去质子化导致入口的开放和出口的关闭,导致从挤压状态过渡到进入状态。AcrB的porter结构域的结构变化与跨膜结构域的质子易位化学计量学密切相关。此外,我们的模拟支持AcrB在无衬底情况下应该采用对称静息状态的假设。
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来源期刊
Molecular BioSystems
Molecular BioSystems 生物-生化与分子生物学
CiteScore
2.94
自引率
0.00%
发文量
0
审稿时长
2.6 months
期刊介绍: Molecular Omics publishes molecular level experimental and bioinformatics research in the -omics sciences, including genomics, proteomics, transcriptomics and metabolomics. We will also welcome multidisciplinary papers presenting studies combining different types of omics, or the interface of omics and other fields such as systems biology or chemical biology.
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