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在原子细胞质模拟中酶铰链弯曲景观中的亚稳态。

Metastable States in the Hinge-Bending Landscape of an Enzyme in an Atomistic Cytoplasm Simulation.

机构信息

Department of Chemistry, University of Illinois Urbana-Champaign, Urbana, Illinois 61801, United States.

Department of Physics, University of Illinois Urbana-Champaign, Urbana, Illinois 61801, United States.

出版信息

J Phys Chem Lett. 2024 Feb 1;15(4):940-946. doi: 10.1021/acs.jpclett.3c03134. Epub 2024 Jan 22.

Abstract

Many enzymes undergo major conformational changes to function in cells, particularly when they bind to more than one substrate. We quantify the large-amplitude hinge-bending landscape of human phosphoglycerate kinase (PGK) in a human cytoplasm. Approximately 70 μs of all-atom simulations, upon coarse graining, reveal three metastable states of PGK with different hinge angle distributions and additional substates. The "open" state was more populated than the "semi-open" or "closed" states. In addition to free energies and barriers within the landscape, we characterized the average transition state passage time of ≈0.3 μs and reversible substrate and product binding. Human PGK in a dilute solution simulation shows a transition directly from the open to closed states, in agreement with previous SAXS experiments, suggesting that the cell-like model environment promotes stability of the human PGK semi-open state. Yeast PGK also sampled three metastable states within the cytoplasm model, with the closed state favored in our simulation.

摘要

许多酶在细胞中发挥作用时会经历重大的构象变化,尤其是当它们结合不止一个底物时。我们在人类细胞质中定量研究了人磷酸甘油酸激酶 (PGK) 的大振幅铰链弯曲景观。经过粗粒化处理,大约 70 μs 的全原子模拟揭示了 PGK 的三种具有不同铰链角度分布和附加亚稳态的亚稳定状态。“打开”状态比“半开”或“关闭”状态更为普遍。除了景观内的自由能和势垒外,我们还表征了平均过渡态通过时间约为 0.3 μs 和可逆的底物和产物结合。在稀溶液模拟中,人 PGK 直接从打开状态过渡到关闭状态,与先前的 SAXS 实验一致,这表明类似细胞的模型环境促进了人 PGK 半开状态的稳定性。酵母 PGK 也在细胞质模型中采样了三个亚稳定状态,我们的模拟中更倾向于关闭状态。

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