首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Evaluation of new generation Salmonella enterica serovar Typhimurium vaccines with regulated delayed attenuation to induce immune responses against PspA
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Evaluation of new generation Salmonella enterica serovar Typhimurium vaccines with regulated delayed attenuation to induce immune responses against PspA

机译:调节延迟减毒以诱导针对PspA的免疫反应的新一代沙门氏沙门氏菌鼠伤寒疫苗的评估

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摘要

Increasing the immunogenicity to delivered antigens by recombinant attenuated Salmonella vaccines (RASV) has been the subject of intensive study. With this goal in mind, we have designed and constructed a new generation of RASV that exhibit regulated delayed attenuation. These vaccine strains are phenotypically wild type at the time of immunization and become attenuated after colonization of host tissues. The vaccine strains are grown under conditions that allow expression of genes required for optimal invasion and colonization of host tissues. Once established in the host, these virulence genes are turned off, fully attenuating the vaccine strain. In this study, we compared 2 of our newly developed regulated delayed attenuation Salmonella enterica serovar Typhimurium strains χ9088 and χ9558 with the Δcya Δcrp Δasd strain χ8133, for their abilities to express and present a secreted form of the α-helical region of pneumococcal surface protein A (PspA) to the mouse immune system. All 3 strains induced high levels of serum antibodies specific for PspA as well as to Salmonella antigens in orally immunized mice. However, both RASVs expressing delayed attenuation elicited significantly greater anti-PspA immune responses, including serum IgG and T cell secretion of IL-4 and IFN-γ, than other groups. Also, vaccination with delayed attenuation strains resulted in a greater degree of protection against Streptococcus pneumoniae challenge than in mice vaccinated with χ8133 (71–86% vs. 21% survival, P ≤ 0.006). Together, the results demonstrate that the regulated attenuation strategy results in highly immunogenic antigen delivery vectors for oral vaccination.
机译:通过重组减毒沙门氏菌疫苗(RASV)提高对递送抗原的免疫原性已成为深入研究的主题。出于这个目标,我们设计并构建了具有可调节延迟衰减的新一代RASV。这些疫苗株在免疫时是表型上的野生型,并且在宿主组织定殖后变得减毒。疫苗株在允许表达宿主组织最佳侵袭和定植所需基因的条件下生长。一旦在宿主中建立,这些毒力基因就会关闭,从而完全减弱疫苗株。在这项研究中,我们比较了我们新开发的2例调节后的延迟减毒肠小肠沙门氏菌鼠伤寒沙门氏菌菌株χ9088和χ9558与ΔcyaΔcrpΔasd菌株χ8133的表达和表达肺炎球菌表面蛋白α螺旋区分泌形式的能力。小鼠免疫系统的(PspA)。在口服免疫的小鼠中,所有3种菌株均诱导高水平的对PspA以及沙门氏菌抗原具有特异性的血清抗体。但是,两种表达延迟减毒的RASVs引起的抗PspA免疫应答均明显高于其他组,包括血清IgG和IL-4和IFN-γ的T细胞分泌。同样,与减毒株相比,接种减毒慢毒株的疫苗对肺炎链球菌攻击的保护程度更高(71-86%对21%的存活率,P≤0.006)。在一起,结果表明,调节的减毒策略导致了用于口服疫苗的高免疫原性抗原递送载体。

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