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Cryo-EM structures of lipopolysaccharide transporter LptB2FGC in lipopolysaccharide or AMP-PNP-bound states reveal its transport mechanism

机译:脂多糖或AMP-PNP约束状态脂多糖转运蛋白LPTB2FGC的Cryo-EM结构揭示了其运输机制

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Lipopolysaccharides (LPS) of Gram-negative bacteria are critical for the defence against cytotoxic substances and must be transported from the inner membrane?(IM) to the outer membrane?(OM) through a bridge formed by seven membrane proteins (LptBFGCADE). The IM component LptBsub2/subFG powers the process through a yet unclarified mechanism. Here we report three high-resolution cryo-EM structures of LptBsub2/subFG alone and complexed with LptC (LptBsub2/subFGC), trapped in either the LPS- or AMP-PNP-bound state. The structures reveal conformational changes between these states and substrate binding with or without LptC. We identify two functional transmembrane arginine-containing loops interacting with the bound AMP-PNP and elucidate allosteric communications between the domains. AMP-PNP binding induces an inward rotation and shift of the transmembrane helices of LptFG and LptC to tighten the cavity, with the closure of two lateral gates, to eventually expel LPS into the bridge. Functional assays reveal the functionality of the LptF and LptG periplasmic domains. Our findings shed light on the LPS transport mechanism.
机译:革兰氏阴性细菌的脂多糖(LPS)对于防御细胞毒性物质是至关重要的,并且必须通过由七膜蛋白(LPTBFGCADE)形成的桥梁从内膜α(IM)输送到外膜α(OM)。 IM组件LPTB 2 FG通过尚未均匀的机制为该过程供电。在这里,我们报告了三种高分辨率的LPTB 2 FG的高分辨率冷冻EM结构,并用LPTC(LPTB 2 FGC)复合,被困在LPS-或AMP-PNP中 - 排行状态。该结构揭示了这些状态与底物结合或不含LPTC之间的构象变化。我们鉴定了与结合的AMP-PNP相互作用的含有两种含有跨膜精氨酸的环,并阐明了域之间的变构通信。 AMP-PNP绑定引起LPTFG和LPTC的透气后螺旋的向内旋转和偏移,以拧紧腔,闭合两个横向栅极,最终将LPS排出到桥中。功能测定揭示了LPTF和LPTG周质域的功能。我们的调查结果在LPS运输机制上阐明了光线。

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