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全长 WzmWzt ABC 转运蛋白的冷冻电镜结构,该转运蛋白用于脂连接的 O 抗原运输。

Cryo-EM structure of the full-length WzmWzt ABC transporter required for lipid-linked O antigen transport.

机构信息

Molecular Physiology and Biological Physics, University of Virginia School of Medicine, Charlottesville, VA 22908.

Molecular Physiology and Biological Physics, University of Virginia School of Medicine, Charlottesville, VA 22908

出版信息

Proc Natl Acad Sci U S A. 2021 Jan 5;118(1). doi: 10.1073/pnas.2016144118. Epub 2020 Dec 21.

Abstract

O antigens are important cell surface polysaccharides in gram-negative bacteria where they extend core lipopolysaccharides in the extracellular leaflet of the outer membrane. O antigen structures are serotype specific and form extended cell surface barriers endowing many pathogens with survival benefits. In the ABC transporter-dependent biosynthesis pathway, O antigens are assembled on the cytosolic side of the inner membrane on a lipid anchor and reoriented to the periplasmic leaflet by the channel-forming WzmWzt ABC transporter for ligation to the core lipopolysaccharides. In many cases, this process depends on the chemical modification of the O antigen's nonreducing terminus, sensed by WzmWzt via a carbohydrate-binding domain (CBD) that extends its nucleotide-binding domain (NBD). Here, we provide the cryo-electron microscopy structure of the full-length WzmWzt transporter from bound to adenosine triphosphate (ATP) and in a lipid environment, revealing a highly asymmetric transporter organization. The CBDs dimerize and associate with only one NBD. Conserved loops at the CBD dimer interface straddle a conserved peripheral NBD helix. The CBD dimer is oriented perpendicularly to the NBDs and its putative ligand-binding sites face the transporter to likely modulate ATPase activity upon O antigen binding. Further, our structure reveals a closed WzmWzt conformation in which an aromatic belt near the periplasmic channel exit seals the transporter in a resting, ATP-bound state. The sealed transmembrane channel is asymmetric, with one open and one closed cytosolic and periplasmic portal. The structure provides important insights into O antigen recruitment to and translocation by WzmWzt and related ABC transporters.

摘要

O 抗原是革兰氏阴性菌细胞表面的重要多糖,它们在外膜的细胞外叶延伸核心脂多糖。O 抗原结构具有血清型特异性,并形成延伸的细胞表面屏障,使许多病原体具有生存优势。在 ABC 转运蛋白依赖的生物合成途径中,O 抗原在内膜的细胞质侧组装在脂质锚上,并通过形成通道的 WzmWzt ABC 转运蛋白重新定向到周质叶,以便与核心脂多糖连接。在许多情况下,这个过程取决于 O 抗原非还原末端的化学修饰,WzmWzt 通过延伸其核苷酸结合域 (NBD) 的碳水化合物结合域 (CBD) 来感知这种修饰。在这里,我们提供了全长 WzmWzt 转运蛋白与 ATP 结合并处于脂质环境中的冷冻电子显微镜结构,揭示了高度不对称的转运蛋白组织。CBD 二聚体化并与仅一个 NBD 相关联。在 CBD 二聚体界面上保守的环跨越保守的外周 NBD 螺旋。CBD 二聚体垂直于 NBD 定向,其假定的配体结合位点面向转运蛋白,可能在 O 抗原结合时调节 ATP 酶活性。此外,我们的结构揭示了一个封闭的 WzmWzt 构象,其中周质通道出口附近的芳香带将转运蛋白密封在休息状态的 ATP 结合状态下。封闭的跨膜通道是不对称的,一个细胞质和周质门户打开,另一个关闭。该结构为 O 抗原与 WzmWzt 及相关 ABC 转运蛋白的募集和易位提供了重要的见解。

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