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来自流感嗜血杆菌伊根菌株 lgtC 突变体的主要 Hex4 脂多糖糖型的结构解析。

Structural elucidation of the major Hex4 lipopolysaccharide glycoform from the lgtC mutant of Haemophilus influenzae strain Eagan.

作者信息

Masoud Hussein, Moxon E Richard, Richards James C

机构信息

Institute for Biological Sciences, National Research Council of Canada, Ottawa, Ontario, Canada K1A 0R6.

出版信息

Carbohydr Res. 2008 Jul 7;343(9):1424-34. doi: 10.1016/j.carres.2008.04.002. Epub 2008 Apr 7.

DOI:10.1016/j.carres.2008.04.002
PMID:18455154
Abstract

Lipopolysaccharide (LPS) oligosaccharide epitopes are major virulence factors of Haemophilus influenzae. The structure of LPS glycoforms of H. influenzae type b strain Eagan containing a mutation in the gene lgtC is investigated. LgtC is involved in the biosynthesis of globoside trisaccharide [alpha-D-Galp-(1-->4)-beta-d-Galp-(1-->4)-beta-D-Glcp-(1-->], an LPS epitope implicated in the virulence of this organism. Glycose and methylation analyses provided information on the composition while electrospray ionization mass spectrometry (ESI-MS) on O-deacylated LPS (LPS-OH) indicated the major glycoform to contain 4 hexoses attached to the common H. influenzae triheptosyl inner-core unit. The structure of the Hex4 glycoform in LPS-OH and core oligosaccharide samples was determined by NMR. It consists of an l-alpha-D-HepIIIp-(1-->2)-[PEtn-->6]-l-alpha-D-HepIIp-(1-->3)-l-alpha-D-HepIp-(1-->5)-[P-->4]-alpha-D-Kdop-(2--> to which a beta-D-Glcp-(1-->4)-alpha-D-Glcp disaccharide unit is extended from HepII at the C-3 position, while HepI and HepIII are substituted at the C-4 and C-2 positions with beta-D-Glcp and beta-D-Galp, respectively. This structure corresponds to that expressed as a subpopulation in the parent strain. 31P NMR studies permitted the identification of subpopulations of LPS containing Kdo substituted at the C-4 position with monophosphate or pyrophosphoethanolamine (PPEtn). HepIII was found to be substituted with either phosphate at the C-4 position or acetate at the C-3 position, but not both of them together in the same subpopulation. The subpopulations containing phosphate and acetate at HepIII and their location have not previously been reported.

摘要

脂多糖(LPS)寡糖表位是流感嗜血杆菌的主要毒力因子。对b型流感嗜血杆菌伊根菌株中lgtC基因发生突变的LPS糖型结构进行了研究。LgtC参与了球苷三糖[α-D-半乳糖-(1→4)-β-D-半乳糖-(1→4)-β-D-葡萄糖-(1→]的生物合成,该LPS表位与该生物体的毒力有关。糖基分析和甲基化分析提供了组成信息,而对O-脱酰化LPS(LPS-OH)的电喷雾电离质谱(ESI-MS)表明,主要糖型含有连接在常见的流感嗜血杆菌三庚糖基内核单元上的4个己糖。通过核磁共振确定了LPS-OH和核心寡糖样品中Hex4糖型的结构。它由一个l-α-D-庚糖III磷酸酯-(1→2)-[磷酰乙醇胺→6]-l-α-D-庚糖II磷酸酯-(1→3)-l-α-D-庚糖I磷酸酯-(1→5)-[磷酸→4]-α-D-酮脱氧辛酮酸-(2→组成,一个β-D-葡萄糖-(1→4)-α-D-葡萄糖二糖单元从庚糖II在C-3位置延伸,而庚糖I和庚糖III分别在C-4和C-2位置被β-D-葡萄糖和β-D-半乳糖取代。该结构与亲本菌株中作为亚群表达的结构相对应。31P核磁共振研究允许鉴定在C-4位置被单磷酸或焦磷酸乙醇胺(PPEtn)取代的含Kdo的LPS亚群。发现庚糖III在C-4位置被磷酸取代或在C-3位置被乙酸取代,但在同一亚群中不会同时被两者取代。此前尚未报道在庚糖III处含有磷酸和乙酸的亚群及其位置。

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