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Topological investigations of the FomA porin from Fusobacterium nucleatum and identification of the constriction loop L6

机译:来自Fusobacterium核心核心核心的拓扑调查,并对收缩环L6鉴定

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Porin FomA in the outer membrane of Fusobacterium nucleatum is a trimeric protein, which exhibits permeability properties similar to that of the well-known enterobacterial diffusion porins. The proposed topology model of the FomA monomer depicts the β-barrel motif typical of diffusion porins, consisting of 16 antiparallel β-strands. To investigate the accuracy of the FomA model and assess the topological relationship with other porins, individual deletions of variable size in seven of the eight surface-exposed regions of the porin were genetically engineered. Deletions in the predicted loops L1 to L7 were tolerated by the FomA porins, as judged by a normal assembly in the outer membrane of Escherichia coli and a sustained pore-forming ability. Deletions in the largest proposed external region, loop L6, made the FomA porins considerably more permeable to antibiotics, indicating larger pore channels. The distinctly increased uptake rates and size exclusion limits displayed by the L6 deletion mutant porins, suggest that loop L6 folds back into the β-barrel thereby constricting the native FomA channel. Thus, the position of the channel constriction loop appears to be shifted towards the C terminus in the FomA porin, as compared to the crystal structures of five non-specific diffusion porins.
机译:Fusobacterium核心内的外膜中的孔隙荧光度是三聚体蛋白质,其具有类似于众所周知的肠杆菌扩散悬蛋白的渗透性。富马单体的所提出的拓扑模型描绘了典型的扩散孔隙的β-桶基序,由16个反平行β-股。为了调查烟雾模型的准确性并评估与其他植物的拓扑关系,散流度八个表面暴露区域中的七个的可变大小的单独缺失是遗传工程化的。通过富马孔脉,通过在大肠杆菌的外膜和持续的孔形成能力中判断预测的环L1至L7中的缺失。在最大提出的外部区域,环L6中删除使FOMA孔隙能够更加渗透到抗生素,表明孔隙较大。 L6缺失突变孔瓣显示的显着增加的摄取速率和尺寸排除限制,表明环L6折叠回β-筒,从而收缩天然吸烟量通道。因此,与五种非特异性扩散孔隙的晶体结构相比,通道收缩回路的位置似乎朝向FOMA孔隙中的C末端移位。

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