Structural basis of lipopolysaccharide maturation by the O-antigen ligase

周质间隙 化学 DNA连接酶 生物化学 细菌外膜 脂多糖 低温电子显微 蛋白质结构 生物物理学 生物 DNA 大肠杆菌 基因 内分泌学
作者
Ashraf KU,Rie Nygaard,Owen N. Vickery,Satchal K. Erramilli,Carmen M. Herrera,Thomas H. McConville,Vasileios I. Petrou,Sabrina I. Giacometti,Meagan Belcher Dufrisne,Kamil Nosol,Allen P Zinkle,Chris L. B. Graham,Michael Loukeris,Brian Kloss,Karolina Skorupińska-Tudek,Ewa Świeżewska,David I. Roper,Oliver B Clarke,Anne‐Catrin Uhlemann,Anthony A. Kossiakoff,M Stephen Trent,Phillip J. Stansfeld,Filippo Mancia
出处
期刊:Nature [Springer Nature]
卷期号:604 (7905): 371-376 被引量:17
标识
DOI:10.1038/s41586-022-04555-x
摘要

The outer membrane of Gram-negative bacteria has an external leaflet that is largely composed of lipopolysaccharide, which provides a selective permeation barrier, particularly against antimicrobials1. The final and crucial step in the biosynthesis of lipopolysaccharide is the addition of a species-dependent O-antigen to the lipid A core oligosaccharide, which is catalysed by the O-antigen ligase WaaL2. Here we present structures of WaaL from Cupriavidus metallidurans, both in the apo state and in complex with its lipid carrier undecaprenyl pyrophosphate, determined by single-particle cryo-electron microscopy. The structures reveal that WaaL comprises 12 transmembrane helices and a predominantly α-helical periplasmic region, which we show contains many of the conserved residues that are required for catalysis. We observe a conserved fold within the GT-C family of glycosyltransferases and hypothesize that they have a common mechanism for shuttling the undecaprenyl-based carrier to and from the active site. The structures, combined with genetic, biochemical, bioinformatics and molecular dynamics simulation experiments, offer molecular details on how the ligands come in apposition, and allows us to propose a mechanistic model for catalysis. Together, our work provides a structural basis for lipopolysaccharide maturation in a member of the GT-C superfamily of glycosyltransferases. Cryo-electron microscopy structures of the bacterial O-antigen ligase WaaL, combined with genetics, biochemistry and molecular dynamics simulations, provide insight into the mechanism by which WaaL catalyses the biosynthesis of lipopolysaccharide.
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