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细菌蛋白质糖基化系统中扩展的聚糖多样性与等位基因多态性以及糖基转移酶基因中的最小遗传改变相关。

Extended glycan diversity in a bacterial protein glycosylation system linked to allelic polymorphisms and minimal genetic alterations in a glycosyltransferase gene.

作者信息

Børud Bente, Anonsen Jan Haug, Viburiene Raimonda, Cohen Ellen Hanne, Samuelsen Anne Berit C, Koomey Michael

机构信息

Department of Biosciences, University of Oslo, Oslo, Norway.

出版信息

Mol Microbiol. 2014 Nov;94(3):688-99. doi: 10.1111/mmi.12789. Epub 2014 Sep 29.

Abstract

Glycans manifest in conjunction with the broad spectrum O-linked protein glycosylation in species within the genus Neisseria display intra- and interstrain diversity. Variability in glycan structure and antigenicity are attributable to differences in the content and expression status of glycan synthesis genes. Given the high degree of standing allelic polymorphisms in these genes, the level of glycan diversity may exceed that currently defined. Here, we identify unique protein-associated disaccharide glycoforms that carry N-acetylglucosamine (GlcNAc) at their non-reducing end. This altered structure was correlated with allelic variants of pglH whose product was previously demonstrated to be responsible for the expression of glucose (Glc)-containing disaccharides. Allele comparisons and site-specific mutagenesis showed that the presence of a single residue, alanine at position 303 in place of a glutamine, was sufficient for GlcNAc versus Glc incorporation. Phylogenetic analyses revealed that GlcNAc-containing disaccharides may be widely distributed within the pgl systems of Neisseria particularly in strains of N. meningitidis. Although analogous minimal structural alterations in glycosyltransferases have been documented in association with lipopolysaccharide and capsular polysaccharide variability, this appears to be the first example in which such changes have been implicated in glycan diversification within a bacterial protein glycosylation system.

摘要

在奈瑟菌属物种中,聚糖与广泛的O-连接蛋白糖基化共同表现出菌株内和菌株间的多样性。聚糖结构和抗原性的变异性归因于聚糖合成基因的含量和表达状态的差异。鉴于这些基因中存在高度的等位基因多态性,聚糖多样性水平可能超过目前所定义的水平。在这里,我们鉴定出了独特的与蛋白质相关的二糖糖型,它们在非还原端携带N-乙酰葡糖胺(GlcNAc)。这种结构改变与pglH的等位基因变体相关,其产物先前已被证明负责含葡萄糖(Glc)二糖的表达。等位基因比较和位点特异性诱变表明,单个残基,即303位的丙氨酸代替谷氨酰胺,足以使GlcNAc与Glc掺入。系统发育分析表明,含GlcNAc的二糖可能广泛分布于奈瑟菌的pgl系统中,尤其是在脑膜炎奈瑟菌菌株中。尽管在脂多糖和荚膜多糖变异性方面已记录了糖基转移酶中类似的最小结构改变,但这似乎是第一个此类变化与细菌蛋白糖基化系统内聚糖多样化有关的例子。

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