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由wbmE编码的一种新型周质酶对支气管败血波氏杆菌O多糖进行组装后修饰。

Post-assembly modification of Bordetella bronchiseptica O polysaccharide by a novel periplasmic enzyme encoded by wbmE.

作者信息

King Jerry D, Vinogradov Evgeny, Preston Andrew, Li Jianjun, Maskell Duncan J

机构信息

Department of Veterinary Medicine, University of Cambridge, Cambridge CB3 0ES, United Kingdom.

出版信息

J Biol Chem. 2009 Jan 16;284(3):1474-83. doi: 10.1074/jbc.M807729200. Epub 2008 Nov 17.

Abstract

Bordetella bronchiseptica is a pathogen of humans and animals that colonizes the respiratory tract. It produces a lipopolysaccharide O antigen that contains a homopolymer of 2,3-dideoxy-2,3-diacetamido-L-galacturonic acid (L-GalNAc3NAcA). Some of these sugars are found in the uronamide form (L-GalNAc3NAcAN), and there is no discernible pattern in the distribution of amides along the chain. A B. bronchiseptica wbmE mutant expresses an O polysaccharide unusually rich in uronamides. The WbmE protein localizes to the periplasm and catalyzes the deamidation of uronamide-rich O chains in lipopolysaccharide purified from the mutant, to attain a wild-type uronamide/uronic acid ratio. WbmE is a member of the papain-like transglutaminase superfamily, and this categorization is consistent with a deamidase role. The periplasmic location of WbmE and its acceptance of complete lipopolysaccharide as substrate indicate that it operates at a late stage in lipopolysaccharide biosynthesis, after polymerization and export of the O chain from the cytoplasm. This is the first report of such a modification of O antigen after assembly. The expression of wbmE is controlled by the Bordetella virulence gene two-component regulatory system, BvgAS, suggesting that this deamidation is a novel mechanism by which these bacteria modify their cell surface charge in response to environmental stimuli.

摘要

支气管败血波氏杆菌是一种定殖于呼吸道的人和动物病原体。它产生一种脂多糖O抗原,该抗原含有2,3 - 二脱氧 - 2,3 - 二乙酰氨基 - L - 半乳糖醛酸(L - GalNAc3NAcA)的同聚物。这些糖中的一些以尿酰胺形式(L - GalNAc3NAcAN)存在,并且酰胺沿链的分布没有明显模式。支气管败血波氏杆菌wbmE突变体表达一种异常富含尿酰胺的O多糖。WbmE蛋白定位于周质,并催化从突变体中纯化的脂多糖中富含尿酰胺的O链的脱酰胺作用,以达到野生型尿酰胺/糖醛酸比例。WbmE是木瓜蛋白酶样转谷氨酰胺酶超家族的成员,这种分类与脱酰胺酶的作用一致。WbmE的周质定位及其对完整脂多糖作为底物的接受表明它在脂多糖生物合成的后期起作用,即在O链从细胞质聚合和输出之后。这是关于O抗原组装后这种修饰的首次报道。wbmE的表达受波氏杆菌毒力基因双组分调节系统BvgAS控制,这表明这种脱酰胺作用是这些细菌响应环境刺激改变其细胞表面电荷的一种新机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fbf3/2615507/d18834236564/zbc0070963990001.jpg

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