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Glycoconjugate vaccine strategies for protection against invasive Salmonella infections.

机译:糖缀合物疫苗策略可预防沙门氏菌感染。

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Salmonella enterica serovars Typhi and Paratyphi A and B and certain non-typhoidal Salmonella enterica (NTS) serovars are important causes of invasive Salmonella disease worldwide. NTS serovars Typhimurium and Enteritidis typically cause gastroenteritis in healthy children and adults in industrialized countries but in certain hosts (e.g., young infants, the elderly, immunocompromised individuals) they also cause invasive infections. These two serovars also cause invasive disease in infants and young children in sub-Saharan Africa. Whereas Salmonella surface polysaccharides are poor immunogens in animal models and do not generate immunologic memory, conjugation with carrier proteins overcomes these limitations. S. Typhi expresses a Vi polysaccharide capsule; Vi either alone or as a glycoconjugate protects humans from typhoid fever. In contrast, S. Paratyphi A and B and NTS (with rare exceptions) do not express capsular polysaccharides. Rather, their surface polysaccharides are the O polysaccharide (OPS) of lipopolysaccharide. In animal studies, immunization with Salmonella COPS (core polysaccharide-OPS) conjugated with carrier proteins generates functional immunity and protects against fatal Salmonella challenge. Conjugating to Salmonella proteins (flagellin, porins) may extend immune responses to another relevant target for antibody generation and enhance the glyconjugate's efficacy.
机译:伤寒沙门氏菌伤寒沙门氏菌和副伤寒A和B以及某些非伤寒性肠炎沙门氏菌(NTS)沙门氏菌是全世界侵袭性沙门氏菌病的重要原因。 NTS鼠伤寒和肠炎沙门氏菌通常会在工业化国家的健康儿童和成人中引起肠胃炎,但在某些宿主(例如,婴儿,老年人,免疫功能低下的人)中,它们也会引起侵袭性感染。这两种血清型还导致撒哈拉以南非洲的婴幼儿侵袭性疾病。沙门氏菌表面多糖在动物模型中是较弱的免疫原,不会产生免疫记忆,而与载体蛋白的结合克服了这些限制。伤寒沙门氏菌表达Vi多糖胶囊;单独或作为糖缀合物的Vi保护人免于伤寒。相反,副伤寒沙门氏菌A和B和NTS(极少数例外)不表达荚膜多糖。而是,它们的表面多糖是脂多糖的O多糖(OPS)。在动物研究中,沙门氏菌COPS(核心多糖-OPS)与载体蛋白结合免疫可产生功能性免疫力,并能抵抗致命的沙门氏菌攻击。与沙门氏菌蛋白(鞭毛蛋白,孔蛋白)结合可将免疫反应扩展至另一个相关靶标,以产生抗体并增强糖缀合物的功效。

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