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Mucosal-Pull Induction of Lung-Resident Memory CD8 T Cells in Parenteral TB Vaccine-Primed Hosts Requires Cognate Antigens and CD4 T Cells

机译:肠外结核疫苗接种宿主中常驻肺记忆CD8 T细胞的粘膜拉动诱导需要同源抗原和CD4 T细胞

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摘要

Tissue-resident memory T cells (TRM) are critical to host defense at mucosal tissue sites. However, the parenteral route of immunization as the most commonly used immunization route in practice is not effective in inducing mucosal TRM cells particularly in the lung. While various respiratory mucosal (RM)-pull strategies are exploited to mobilize parenteral vaccine-primed T cells into the lung, whether such RM-pull strategies can all or differentially induce Ag-specific TRM cells in the lung remains unclear. Here, we have addressed this issue by using a parenteral TB vaccine-primed and RM-pull model. We show that both Ag-independent and Ag-dependent RM-pull strategies are able to mobilize Ag-specific CD8 T cells into the lung. However, only the RM-pull strategy with cognate antigens can induce robust Ag-specific CD8 TRM cells in the lung. We also show that the cognate Ag-based RM-pull strategy is the most effective in inducing TRM cells when carried out during the memory phase, as opposed to the effector phase, of T cell responses to parenteral prime vaccination. We further find that cognate Ag-induced CD4 T cells play an important role in the development of CD8 TRM cells in the lung. Our study holds implications in developing effective vaccine strategies against respiratory pathogens.
机译:组织驻留记忆T细胞(TRM)对于黏膜组织部位的宿主防御至关重要。但是,作为实践中最常用的免疫途径的肠胃外免疫途径在诱导粘膜TRM细胞尤其是肺中不起作用。尽管利用了各种呼吸道粘膜(RM)拉动策略将肠胃外疫苗引发的T细胞动员到肺中,但是这种RM拉动策略是否可以全部或差异诱导肺中的Ag特异性TRM细胞仍不清楚。在这里,我们通过使用肠胃外结核病疫苗引发的RM拉模型解决了这个问题。我们表明,既不依赖于银又依赖于银的RM-拉策略能够将银特异性CD8 T细胞动员到肺中。但是,只有具有同源抗原的RM拉策略才能在肺中诱导健壮的Ag特异性CD8 TRM细胞。我们还显示,基于Ag的同源RM拉策略在诱导肠外疫苗接种的T细胞应答的记忆阶段(而不是效应阶段)期间最有效地诱导TRM细胞。我们进一步发现,同源银诱导的CD4 T细胞在肺中CD8 TRM细胞的发育中起重要作用。我们的研究对开发针对呼吸道病原体的有效疫苗策略具有重要意义。

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