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Conformational states and association mechanism of Yersinia pestis Caf1 subunits.

机译:鼠疫耶尔森菌Caf1亚基的构象状态和缔合机制。

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Bacterial infectivity often relies on efficient attachment to the host cells through adhesive extensions. Unveiling the structural basis of the formation of these organelles is of paramount importance for both academic and applicative implications. Computational approaches may fruitfully complement experimental studies by providing information on specific conformational states whose characterization is difficult. Here, we report molecular dynamics characterizations of Yersinia pestis Caf1 subunit in its monomeric-unbound and dimeric states. Data on the monomeric form indicate that it is highly reactive and evolves toward compact states, which likely hamper subunit-subunit association. In line with recent experimental reports, this finding implies that chaperone release and subunit-subunit association must be simultaneous. MD analysis on Caf1 dimer lead to the formation of a novel assembly endowed with a significant stability in the simulation timescale. Using these data, an end-to-end model of the fiber, which well agrees with available experimental data, was also generated.
机译:细菌的感染力通常依赖于通过黏附剂延伸与宿主细胞的有效结合。揭开这些细胞器形成的结构基础对于学术和应用意义都至关重要。计算方法可以通过提供表征困难的特定构象状态的信息来对实验研究进行有益的补充。在这里,我们报告鼠疫耶尔森氏菌Caf1亚基在其单体未结合和二聚体状态的分子动力学表征。单体形式的数据表明它具有很高的反应性,并向紧密状态发展,这可能会阻碍亚基-亚基的缔合。与最近的实验报告一致,该发现暗示伴侣分子释放和亚基-亚基缔合必须同时进行。对Caf1二聚体的MD分析导致形成新颖的装配,该装配在仿真时标上具有显着的稳定性。使用这些数据,还生成了与可用的实验数据完全吻合的光纤的端到端模型。

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