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人类和恒河猴对9V型肺炎链球菌荚膜多糖主链和O-乙酰侧链的抗体反应。

Antibody responses to capsular polysaccharide backbone and O-acetate side groups of Streptococcus pneumoniae type 9V in humans and rhesus macaques.

作者信息

McNeely T B, Staub J M, Rusk C M, Blum M J, Donnelly J J

机构信息

Departments of Virus and Cell Biology, Merck Research Laboratories, West Point, Pennsylvania, USA.

出版信息

Infect Immun. 1998 Aug;66(8):3705-10. doi: 10.1128/IAI.66.8.3705-3710.1998.

Abstract

Streptococcus pneumoniae is responsible for high rates of pneumococcal bacteremia, meningitis, pneumonia, and acute otitis media worldwide. Protection from disease is conferred by antibodies specific for the polysaccharide (Ps) capsule of the bacteria. Of the four types of group 9 pneumococci, types 9N and 9V cause the most disease, and both types are included in the polyvalent pneumococcal vaccine. The type 9V capsule consists of repeating pentasaccharide units linearly arranged, with an average of 1 to 2 mol of O-acetate side chains per mol of repeat units, added in a complex pattern in which not all repeat units are alike. alpha-GlcA residues may be O-acetylated in the 2 (17%) or 3 (25%) position and beta-ManNAc residues may be O-acetylated in the 4 (6%) or 6 (55%) position. Under certain conditions, the O-acetate side chains are subject to oxidation, which results in subsequent de-O-acetylation of a significant number of the repeat units. This de-O-acetylation could adversely affect the efficacy of a vaccine containing the 9V Ps. A study was undertaken to compare the relative contributions of O-acetate and Ps backbone epitopes in the immune response to S. pneumoniae 9V type-specific Ps. In both an infant rhesus monkey model and humans, antibodies against the non-O-acetylated 9V backbone as well as against O-acetylated 9V Ps were detected. Functional (opsonophagocytic) activity was observed in antisera in which the predominant species of antibody recognized de-O-acetylated 9V Ps. We concluded that the O-acetate side groups, while recognized, are not essential to the ability of the 9V Ps to induce functional antibody responses.

摘要

肺炎链球菌在全球范围内导致了高发病率的肺炎球菌菌血症、脑膜炎、肺炎和急性中耳炎。针对该细菌多糖(Ps)荚膜的特异性抗体可提供疾病保护。在9型肺炎球菌的四种类型中,9N型和9V型引起的疾病最多,这两种类型都包含在多价肺炎球菌疫苗中。9V型荚膜由线性排列的重复五糖单元组成,每摩尔重复单元平均含有1至2摩尔的O - 乙酰侧链,其添加方式复杂,并非所有重复单元都相同。α - GlcA残基可能在2位(17%)或3位(25%)被O - 乙酰化,β - ManNAc残基可能在4位(6%)或6位(55%)被O - 乙酰化。在某些条件下,O - 乙酰侧链会发生氧化,这会导致大量重复单元随后发生脱O - 乙酰化。这种脱O - 乙酰化可能会对含有9V Ps的疫苗效力产生不利影响。开展了一项研究,以比较O - 乙酰基和Ps主链表位在针对肺炎链球菌9V型特异性Ps的免疫反应中的相对贡献。在恒河猴幼猴模型和人类中,均检测到了针对非O - 乙酰化9V主链以及O - 乙酰化9V Ps的抗体。在主要抗体种类识别脱O - 乙酰化9V Ps的抗血清中观察到了功能性(调理吞噬)活性。我们得出结论,O - 乙酰侧基虽然能被识别,但对于9V Ps诱导功能性抗体反应的能力并非必不可少。

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