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准马尔可夫状态模型阐明细菌RNA聚合酶门开放动力学在DNA加载和抗生素抑制中的作用

Role of bacterial RNA polymerase gate opening dynamics in DNA loading and antibiotics inhibition elucidated by quasi-Markov State Model.

作者信息

Unarta Ilona Christy, Cao Siqin, Kubo Shintaroh, Wang Wei, Cheung Peter Pak-Hang, Gao Xin, Takada Shoji, Huang Xuhui

机构信息

Department of Chemical and Biological Engineering, The Hong Kong University of Science and Technology, Kowloon, Hong Kong.

Center of Systems Biology and Human Health, State Key Laboratory of Molecular Neuroscience, The Hong Kong University of Science and Technology, Kowloon, Hong Kong.

出版信息

Proc Natl Acad Sci U S A. 2021 Apr 27;118(17). doi: 10.1073/pnas.2024324118.

Abstract

To initiate transcription, the holoenzyme (RNA polymerase [RNAP] in complex with σ factor) loads the promoter DNA via the flexible loading gate created by the clamp and β-lobe, yet their roles in DNA loading have not been characterized. We used a quasi-Markov State Model (qMSM) built from extensive molecular dynamics simulations to elucidate the dynamics of holoenzyme's gate opening. We showed that during gate opening, β-lobe oscillates four orders of magnitude faster than the clamp, whose opening depends on the Switch 2's structure. Myxopyronin, an antibiotic that binds to Switch 2, was shown to undergo a conformational selection mechanism to inhibit clamp opening. Importantly, we reveal a critical but undiscovered role of β-lobe, whose opening is sufficient for DNA loading even when the clamp is partially closed. These findings open the opportunity for the development of antibiotics targeting β-lobe of RNAP. Finally, we have shown that our qMSMs, which encode non-Markovian dynamics based on the generalized master equation formalism, hold great potential to be widely applied to study biomolecular dynamics.

摘要

为启动转录,全酶(与σ因子结合的RNA聚合酶[RNAP])通过由夹子和β叶形成的灵活加载门加载启动子DNA,但其在DNA加载中的作用尚未得到表征。我们使用了基于广泛分子动力学模拟构建的准马尔可夫状态模型(qMSM)来阐明全酶门打开的动力学。我们表明,在门打开期间,β叶的振荡速度比夹子快四个数量级,夹子的打开取决于开关2的结构。已证明,与开关2结合的抗生素粘球菌素通过构象选择机制抑制夹子打开。重要的是,我们揭示了β叶一个关键但未被发现的作用,即使夹子部分关闭,其打开也足以进行DNA加载。这些发现为开发靶向RNAPβ叶的抗生素提供了机会。最后,我们表明,我们基于广义主方程形式编码非马尔可夫动力学的qMSM在广泛应用于研究生物分子动力学方面具有巨大潜力。

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