首页> 外文期刊>Clinical and vaccine immunology: CVI >Intranasal vaccination with the recombinant Listeria monocytogenes DeltaactA prfA* mutant elicits robust systemic and pulmonary cellular responses and secretory mucosal IgA.
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Intranasal vaccination with the recombinant Listeria monocytogenes DeltaactA prfA* mutant elicits robust systemic and pulmonary cellular responses and secretory mucosal IgA.

机译:鼻内接种疫苗与重组单核细胞增多性李斯特氏菌DeltaactA prfA *突变抒发健壮的全身和肺细胞和分泌粘膜IgA的反应。

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We previously showed that recombinant (r) Listeria monocytogenes carrying DeltaactA and a selected prfA* mutation (r-Listeria DeltaactA prfA*) secreted >100-fold more immunogen in broth culture than wild-type r-Listeria or r-Listeria DeltaactA and elicited much greater cellular and humoral immune responses than r-Listeria DeltaactA after intravenous vaccination of mice. Here, we conducted comparative studies evaluating vaccine-elicited immune responses in systemic and mucosal sites after intranasal, intravenous, intraperitoneal, or subcutaneous immunization of mice with r-Listeria DeltaactA prfA* vaccine candidates. Intranasal vaccination of mice with r-Listeria DeltaactA prfA* vaccine candidates elicited a robust gamma interferon-positive (IFN-gamma(+)) cellular response in systemic sites, although intravenous or intraperitoneal immunization was more efficient. Surprisingly, intranasal vaccination elicited an appreciable pulmonary IFN-gamma(+) cellular response that was nonstatistically higher than the magnitude induced by the intravenous route but was significantly greater than that elicited by subcutaneous immunization. Furthermore, although intranasal r-Listeria DeltaactA prfA* delivery induced poor systemic IgG responses, intranasal vaccination elicited appreciable secretory immunogen-specific IgA titers that were similar to or higher in mucosal fluid than those induced by subcutaneous and intravenous immunizations. Thus, intranasal vaccination with r-Listeria DeltaactA prfA* appears to be a useful approach for eliciting robust systemic and pulmonary cellular responses and measurable secretory mucosal IgA titers.
机译:我们之前显示,重组(r)李斯特菌monocytogenes携带DeltaactA和选择prfA *突变(r-Listeria DeltaactA prfA *)分泌> 100倍在汤免疫原比野生型r-Listeria或r-Listeria文化DeltaactA和引起细胞和大得多比r-Listeria体液免疫反应DeltaactA后静脉注射疫苗接种的老鼠。在这里,我们评估进行了比较研究疫苗诱导的免疫反应系统鼻内粘膜网站后,静脉注射,腹腔内或皮下免疫的小鼠r-Listeria DeltaactA prfA *疫苗候选人。r-Listeria DeltaactA prfA *候选疫苗引起一个健壮的伽马interferon-positive(IFN-gamma(+))在系统性的细胞反应网站,尽管静脉或腹腔内免疫接种是更有效率。鼻内接种引起可观那是肺IFN-gamma(+)细胞反应nonstatistically高于级但静脉诱导的途径明显大于所引起皮下免疫。鼻内r-Listeria DeltaactA prfA *交货诱导系统性免疫球蛋白反应差,鼻内疫苗接种引起明显的分泌immunogen-specific IgA浓度相似在比诱导粘膜液或更高皮下、静脉注射免疫接种。因此,与r-Listeria鼻内接种疫苗DeltaactA prfA *似乎是一个有用的方法为诱发健壮的系统性和肺分泌细胞反应和可测性粘膜IgA滴度。

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