首页> 美国卫生研究院文献>Infection and Immunity >Synthesis characterization and clinical evaluation of conjugate vaccines composed of the O-specific polysaccharides of Shigella dysenteriae type 1 Shigella flexneri type 2a and Shigella sonnei (Plesiomonas shigelloides) bound to bacterial toxoids.
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Synthesis characterization and clinical evaluation of conjugate vaccines composed of the O-specific polysaccharides of Shigella dysenteriae type 1 Shigella flexneri type 2a and Shigella sonnei (Plesiomonas shigelloides) bound to bacterial toxoids.

机译:痢疾志贺氏菌1型弗氏志贺氏菌2a型和索氏志贺氏菌(Plesiomonas shigelloides)与细菌类毒素结合的O特异性多糖组成的结合疫苗的合成表征和临床评估。

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摘要

The theoretic basis for developing conjugate vaccines, to induce immunoglobulin G (IgG) lipopolysaccharide (LPS) antibodies for the prevention of shigellosis, has been described (J. B. Robbins, C.-Y. Chu, and R. Schneerson, Clin. Infect. Dis. 15:346-361, 1992). The O-specific polysaccharides (O-SPs) of Shigella dysenteriae type 1, S. flexneri type 2a, and S. sonnei were covalently bound to carrier proteins. Alone, the O-SPs were not immunogenic in mice. Conjugates of these O-SPs, injected into young outbred mice subcutaneously as saline solutions containing 2.5 micrograms of saccharide, elicited serum IgG and IgM antibodies with booster responses; adsorption onto alum enhanced their immunogenicity. Injection of 25 micrograms of these conjugates into adult volunteers elicited mild local reactions only. Each conjugate induced a significant rise of the geometric mean serum IgG, IgM, and IgA LPS antibody levels. A second injection 6 weeks later did not elicit booster responses, and adsorption of the conjugates onto alum did not enhance their immunogenicity. Conjugate-induced levels of IgA, but not IgG or IgM, declined to preimmunization levels at day 56. The levels of postimmunization antibodies of the three immunoglobulin classes were similar to or higher than those of recruits in the Israel Defense Force following shigellosis caused by S. flexneri type 2a or S. sonnei. These data provide the basis for evaluating these conjugates to prevent shigellosis.
机译:已经描述了开发偶联疫苗以诱导免疫球蛋白G(IgG)脂多糖(LPS)抗体预防志贺氏菌病的理论基础(JB Robbins,C.-Y. Chu,and R.Schneerson,Clin.Infect。Dis 15:346-361,1992)。痢疾志贺氏菌1型,弗氏链球菌2a型和索内链球菌的O特异性多糖(O-SPs)共价结合到载体蛋白上。单独地,O-SP在小鼠中不是免疫原性的。这些O-SP的结合物以含有2.5微克糖的盐溶液皮下注射到年轻的近交小鼠中,引起血清IgG和IgM抗体增强反应;吸附到明矾上增强了它们的免疫原性。向成年志愿者注射25微克这些结合物只会引起轻微的局部反应。每种缀合物均导致几何平均血清IgG,IgM和IgA LPS抗体水平显着升高。 6周后的第二次注射未引起加强反应,并且缀合物在明矾上的吸附未增强其免疫原性。在第56天,结合物诱导的IgA水平(而非IgG或IgM)降至免疫前水平。三种免疫球蛋白类别的免疫后抗体水平与S引起的志贺氏菌感染后的以色列国防军新兵相似或更高。 。flexneri类型2a或S. sonnei。这些数据为评估这些缀合物预防志贺氏菌病提供了基础。

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