首页> 外文期刊>FEMS immunology and medical microbiology >Genetic detoxification of an aroA Salmonella enterica serovar Typhimurium vaccine strain does not compromise protection against virulent Salmonella and enhances the immune responses towards a protective malarial antigen
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Genetic detoxification of an aroA Salmonella enterica serovar Typhimurium vaccine strain does not compromise protection against virulent Salmonella and enhances the immune responses towards a protective malarial antigen

机译:aroA肠炎沙门氏菌鼠伤寒沙门氏菌疫苗菌株的遗传解毒不影响针对强毒沙门氏菌的保护,并增强了对保护性疟疾抗原的免疫反应

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摘要

Live Salmonella vaccines are limited in use by the inherent toxicity of the lipopolysaccharide. The waaN gene encodes a myristyl transferase required for the secondary acylation of lipid A in lipopolysaccharide. A waaN mutant exhibits reduced induction of the inflammatory cytokines associated with lipopolysaccharide toxicity. Here the characteristics of a Salmonella enterica serovar Typhimurium aroA waaN mutant (SK100) in vitro and in vivo compared with its parent aroA strain (SL3261) were described. Phenotypic analysis of purified lipopolysaccharide obtained from SK100 confirmed that the physical and biological activities of the lipopolysaccharide had been altered. Nevertheless both strains had similar patterns of colonization and persistence in mice and significantly the aroA waaN mutant was equally as effective as the parent at protecting against challenge with wild-type S. Typhimurium. Furthermore, a SK100 strain was constructed expressing both tetanus toxin fragment C and the circumsporozoite protein of a malaria parasite. In marked contrast to its isogenic parent, the new attenuated strain induces significantly enhanced immune responses against the circumsporozoite protein. The waaN mutation enhances the ability of this strain to elicit immune responses towards guest antigens. This study provides important insights into the development of safe and effective multivalent Salmonella vaccines.
机译:沙门氏菌活疫苗的使用受到脂多糖固有毒性的限制。 waaN基因编码脂多糖中脂质A的二次酰化所需的肉豆蔻基转移酶。 waaN突变体显示出与脂多糖毒性相关的炎性细胞因子的诱导减少。在此描述了沙门氏菌血清型鼠伤寒aroA waaN突变体(SK100)与亲本aroA菌株(SL3261)相比的特性。从SK100获得的纯化的脂多糖的表型分析证实,脂多糖的物理和生物学活性已经改变。然而,这两种菌株在小鼠中的定殖和持久性模式相似,并且明显地,aroA waaN突变体在抵抗野生型鼠伤寒沙门氏菌的攻击方面与亲本同样有效。此外,构建了SK100菌株,该菌株表达破伤风毒素片段C和疟原虫的环子孢子蛋白。与它的同基因亲本形成鲜明对比的是,新的减毒株诱导了针对环子孢子蛋白的明显增强的免疫反应。 waaN突变增强了该菌株引发针对客体抗原的免疫反应的能力。这项研究为开发安全有效的多价沙门氏菌疫苗提供了重要的见识。

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