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Francisella tularensis Vaccines Elicit Concurrent Protective T- and B-Cell Immune Responses in BALB/cByJ Mice

机译:图拉弗朗西斯菌疫苗在BALB / cByJ小鼠中同时引起保护性T和B细胞免疫反应

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摘要

In the last decade several new vaccines against Francisella tularensis, which causes tularemia, have been characterized in animal models. Whereas many of these vaccine candidates showed promise, it remains critical to bridge the preclinical studies to human subjects, ideally by taking advantage of correlates of protection. By combining in vitro intramacrophage LVS replication with gene expression data through multivariate analysis, we previously identified and quantified correlative T cell immune responses that discriminate vaccines of different efficacy. Further, using C57BL/6J mice, we demonstrated that the relative levels of gene expression vary according to vaccination route and between cell types from different organs. Here, we extended our studies to the analysis of T cell functions of BALB/cByJ mice to evaluate whether our approach to identify correlates of protection also applies to a Th2 dominant mouse strain. BALB/cByJ mice had higher survival rates than C57BL/6J mice when they were immunized with suboptimal vaccines and challenged. However, splenocytes derived from differentially vaccinated BALB/cByJ mice controlled LVS intramacrophage replication in vitro in a pattern that reflected the hierarchy of protection observed in C57BL/6J mice. In addition, gene expression of selected potential correlates revealed similar patterns in splenocytes of BALB/cByJ and C57BL/6J mice. The different survival patterns were related to B cell functions, not necessarily to specific antibody production, which played an important protective role in BALB/cByJ mice when vaccinated with suboptimal vaccines. Our studies therefore demonstrate the range of mechanisms that operate in the most common mouse strains used for characterization of vaccines against F. tularensis, and illustrate the complexity necessary to define a comprehensive set of correlates.
机译:在过去的十年中,已经在动物模型中鉴定了几种针对土拉弗朗西斯菌的新疫苗,该疫苗可引起土拉菌血症。尽管许多候选疫苗显示出希望,但将临床前研究与人类受试者联系起来仍然至关重要,理想情况下是利用保护相关因素。通过多变量分析将体外巨噬细胞内的LVS复制与基因表达数据结合起来,我们先前鉴定并量化了相关T细胞免疫应答,以区分不同功效的疫苗。此外,使用C57BL / 6J小鼠,我们证明了基因表达的相对水平根据疫苗接种途径以及来自不同器官的细胞类型而变化。在这里,我们将研究扩展到BALB / cByJ小鼠的T细胞功能分析,以评估我们鉴定保护相关性的方法是否也适用于Th2显性小鼠品系。用次优疫苗免疫和攻击后,BALB / cByJ小鼠的存活率高于C57BL / 6J小鼠。但是,衍生自差异接种的BALB / cByJ小鼠的脾细胞在体外控制LVS巨噬细胞内复制的方式反映了在C57BL / 6J小鼠中观察到的保护等级。此外,选定的潜在关联的基因表达揭示了BALB / cByJ和C57BL / 6J小鼠脾细胞中的相似模式。不同的存活方式与B细胞功能有关,而与特异性抗体的产生无关,当接种次优疫苗后,这些抗体在BALB / cByJ小鼠中起着重要的保护作用。因此,我们的研究证明了可用于鉴定抗图拉弗雷特菌疫苗的最常见小鼠品系中发挥作用的机制范围,并阐明了定义一套全面的相关因子所必需的复杂性。

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