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A coevolution-guided model for the rotor of the bacterial flagellar motor

机译:细菌鞭毛马达转子的协同进化模型

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摘要

The Salmonella typhimurium trans-membrane FliF MS ring templates assembly of the rotary bacterial flagellar motor, which also contains a cytoplasmic C-ring. A full-frame fusion of FliF with the rotor protein FliG assembles rings in non-motile expression hosts. 3D electron microscopy reconstructions of these FliFFliG rings show three high electron-density sub-volumes. 3D-classification revealed heterogeneity of the assigned cytoplasmic volume consistent with FliG lability. We used residue coevolution to construct homodimer building blocks for ring assembly, with X-ray crystal structures from other species and injectisome analogs. The coevolution signal validates folds and, importantly, indicates strong homodimer contacts for three ring building motifs (RBMs), initially identified in injectisome structures. It also indicates that the cofolded domains of the FliG N-terminal domain (FliG_N) with embedded α-helical FliF carboxy-terminal tail homo-oligomerize. The FliG middle and C-terminal domains (FliG_MC) have a weak signal for homo-dimerization but have coevolved to conserve their stacking contact. The homodimers and their ring models fit well into the 3D reconstruction. We hypothesize that a stable FliF periplasmic hub provides a platform for FliG ring self-assembly, but the FliG_MC ring has only limited stability without the C-ring. We also present a mechanical model for torque transmission in the FliFFliG ring.
机译:旋转细菌鞭毛马达的鼠伤寒沙门氏菌跨膜FliF MS环模板组件,其中还包含细胞质C环。 FliF与转子蛋白FliG的全帧融合可在非运动性表达宿主中装配环。这些FliFFliG环的3D电子显微镜重建显示了三个高电子密度子体积。 3D分类显示分配的胞质体积的异质性与FliG不稳定性一致。我们使用残基协同进化构建了用于环组装的均二聚体构建基块,并带有来自其他物种和注射体类似物的X射线晶体结构。协同进化信号验证了折叠,并且重要的是,它表明了最初在注射体结构中识别的三个环结构基序(RBM)的强大同二聚体接触。这也表明具有嵌入的α-螺旋FliF羧基末端尾部均聚的FliG N末端结构域(FliG_N)的共折叠域。 FliG中间和C末端域(FliG_MC)的均二聚信号很弱,但共同进化以保持它们的堆叠接触。同型二聚体及其环模型非常适合3D重建。我们假设稳定的FliF周质中心为FliG环的自组装提供了平台,但是FliG_MC环在没有C环的情况下仅具有有限的稳定性。我们还介绍了FliFFliG环中扭矩传递的机械模型。

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