首页> 外文OA文献 >Role of the group B antigen of Streptococcus agalactiae a peptidoglycan-anchored polysaccharide involved in cell wall biogenesis : a Peptidoglycan-Anchored Polysaccharide involved in cell wall biogenesis
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Role of the group B antigen of Streptococcus agalactiae a peptidoglycan-anchored polysaccharide involved in cell wall biogenesis : a Peptidoglycan-Anchored Polysaccharide involved in cell wall biogenesis

机译:无乳链球菌B组抗原的作用与细胞壁生物发生有关的肽聚糖锚定的多糖:与细胞壁生物发生有关的肽聚糖锚定的多糖。

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摘要

Streptococcus agalactiae (Group B streptococcus, GBS) is a leading cause of infections in neonates and an emerging pathogen in adults. The Lancefield Group B carbohydrate (GBC) is a peptidoglycan-anchored antigen that defines this species as a Group B Streptococcus. Despite earlier immunological and biochemical characterizations, the function of this abundant glycopolymer has never been addressed experimentally. Here, we inactivated the gene gbcO encoding a putative UDP-N-acetylglucosamine-1-phosphate:lipi​dphosphate transferase thought to catalyze the first step of GBC synthesis. Indeed, the gbcO mutant was unable to synthesize the GBC polymer, and displayed an important growth defect in vitro. Electron microscopy study of the GBC-depleted strain of S. agalactiae revealed a series of growth-related abnormalities: random placement of septa, defective cell division and separation processes, and aberrant cell morphology. Furthermore, vancomycin labeling and peptidoglycan structure analysis demonstrated that, in the absence of GBC, cells failed to initiate normal PG synthesis and cannot complete polymerization of the murein sacculus. Finally, the subcellular localization of the PG hydrolase PcsB, which has a critical role in cell division of streptococci, was altered in the gbcO mutant. Collectively, these findings show that GBC is an essential component of the cell wall of S. agalactiae whose function is reminiscent of that of conventional wall teichoic acids found in Staphylococcus aureus or Bacillus subtilis. Furthermore, our findings raise the possibility that GBC-like molecules play a major role in the growth of most if not all beta –hemolytic streptococci.
机译:无乳链球菌(B组链球菌,GBS)是新生儿感染的主要原因,并且是成年人中新兴的病原体。 Lancefield B组碳水化合物(GBC)是肽聚糖锚定的抗原,其将该物种定义为B组链球菌。尽管有早期的免疫学和生物化学表征,但是这种丰富的糖聚合物的功能从未通过实验得到解决。在这里,我们灭活了编码推定的UDP-N-乙酰氨基葡糖-1-磷酸:脂二磷酸转移酶的基因gbcO,该酶被认为可以催化GBC合成的第一步。实际上,gbcO突变体无法合成GBC聚合物,并在体外显示出重要的生长缺陷。对无乳链球菌GBC耗尽菌株的电子显微镜研究显示了一系列与生长有关的异常:隔垫的随机放置,缺陷的细胞分裂和分离过程以及异常的细胞形态。此外,万古霉素标记和肽聚糖结构分析表明,在不存在GBC的情况下,细胞无法启动正常的PG合成,并且无法完成水ure素囊的聚合。最后,在gbcO突变体中,PG水解酶PcsB的亚细胞定位在链球菌的细胞分裂中起着关键作用。总的来说,这些发现表明GBC是无乳链球菌细胞壁的重要组成部分,其功能让人联想到在金黄色葡萄球菌或枯草芽孢杆菌中发现的常规壁甲壁酸。此外,我们的发现增加了GBC样分子在大多数(即使不是全部)β-溶血性链球菌生长中起主要作用的可能性。

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