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黏膜共免疫重组乳球菌分泌 vapA 抗原和瘦素的小鼠引发保护性免疫反应,对抗马红球菌感染。

Mucosal co-immunization of mice with recombinant lactococci secreting VapA antigen and leptin elicits a protective immune response against Rhodococcus equi infection.

机构信息

Anses, Dozulé Laboratory for Equine Diseases, Bacteriology and Parasitology Unit, Goustranville, 14430 Dozulé, France.

出版信息

Vaccine. 2011 Dec 9;30(1):95-102. doi: 10.1016/j.vaccine.2011.10.026. Epub 2011 Oct 20.

DOI:10.1016/j.vaccine.2011.10.026
PMID:22019740
Abstract

Rhodococcus equi causes severe pneumonia in foals and has recently gained attention as a significant opportunistic pathogen in immunocompromised humans. However, no effective vaccine to prevent rhodococcosis is currently available. In this study, we have engineered the food-grade bacterium Lactococcus lactis to secrete the virulence-associated protein A from R. equi (LL-VapA). The immunogenic potential of LL-VapA strain was then evaluated after either intragastric or intranasal immunization in mice either alone or in combination with LL-Lep, a recombinant strain of L. lactis secreting biologically active leptin, a pleiotropic hormone with significant immunomodulatory properties. Intragastric administration of LL-VapA led to the highest VapA-specific mucosal response whereas intranasal administration led to the highest systemic immune responses. Cytokines released from in vitro-stimulated spleen cells show both a strong IFN-γ response and an increase of IL-4 level in all immunized groups, except for the group intranasally co-administered with both LL-VapA and LL-Lep. Strikingly, a significant reduction in R. equi viable counts in liver and spleen was observed four days after intravenous challenge with a virulent strain of R. equi in all immunized groups except for the group vaccinated by intragastric route with LL-VapA. Altogether, our results demonstrate that LL-VapA can evoke a T(H)1-based protective immune response in intranasally immunized mice. This response is enhanced when co-administered with LL-Lep strain, whereas only co-administration of LL-VapA and LL-Lep can induce a protective immune response in intragastric vaccinated mice, associated with a T(H)1/T(H)2 cytokine response.

摘要

马红球菌可引起驹肺炎,最近已成为免疫功能低下人群中重要的机会性病原菌而受到关注。然而,目前尚无有效的疫苗来预防马红球菌病。在这项研究中,我们构建了能分泌马红球菌相关毒力蛋白 A(LL-VapA)的食品级乳球菌 lactis。随后,我们通过胃内或鼻腔免疫单独或与分泌具有生物活性瘦素的重组乳球菌 lactis(LL-Lep)的 LL-Lep 联合免疫,评估了 LL-VapA 株的免疫原性。胃内给予 LL-VapA 导致了最高的 VapA 特异性黏膜反应,而鼻腔给予则导致了最高的系统免疫反应。体外刺激脾细胞释放的细胞因子显示,所有免疫组均有强烈的 IFN-γ 反应和 IL-4 水平升高,除了鼻腔联合给予 LL-VapA 和 LL-Lep 的组外。值得注意的是,在静脉内用毒力株 R. equi 攻击后 4 天,所有免疫组的肝和脾中的 R. equi 活菌数均显著减少,除了经胃内途径用 LL-VapA 免疫的组外。总之,我们的结果表明,LL-VapA 可以在鼻腔免疫的小鼠中引发 T(H)1 型保护性免疫应答。与 LL-Lep 株联合给予时,这种应答得到增强,而仅联合给予 LL-VapA 和 LL-Lep 才能在胃内免疫的小鼠中诱导保护性免疫应答,并伴有 T(H)1/T(H)2 细胞因子应答。

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