Recruitment of dendritic cell progenitors to foci of influenza A virus infection sustains immunity

MAR CABEZA-CABRERIZO; CARLOS M. MINUTTI; MARIANA PEREIRA DA COSTA

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Recruitment of dendritic cell progenitors to foci of influenza A virus infection sustains immunity

机译：将树突状细胞祖细胞募集到流感病毒感染的焦点

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Protection from infection with respiratory viruses such as influenza A virus (IAV) requires T cell–mediated immune responses initiated by conventional dendritic cells (cDCs) that reside in the respiratory tract. Here, we show that effective inductionof T cell responses against IAV in mice requires reinforcement of the resident lung cDC network by cDC progenitors. We found that CCR2-binding chemokines produced during IAV infection recruit pre-cDCs from blood and direct them to foci of infection, increasing the number of progeny cDCs next to sites of viral replication. Ablation of CCR2 in the cDC lineage prevented this increase and resulted in a deficit in IAV-specific T cell responses and diminished resistance to reinfection. These data suggest that the homeostatic network of cDCs in tissues is insufficient for immunity and reveal a chemokine-driven mechanism of expansion of lung cDC numbers that amplifies T cell responses against respiratory viruses.

机译：免受流感病毒（IAV）等呼吸道病毒感染的保护需要由常规树突状细胞（CDC）引发的T细胞介导的免疫反应，该反应位于呼吸道中。在这里，我们表明，针对小鼠IAV的T细胞反应的有效诱导需要通过CDC祖细胞加强居民肺CDC网络。我们发现，在IAV感染期间产生的CCR2结合趋化因子从血液中募集了PRECDC，并将其引导到感染焦点，从而增加了病毒复制部位旁边的后代CDC的数量。 CCR2在CDC谱系中的消融阻止了这种增加，并导致IAV特异性T细胞反应的不足和对再感染的耐药性降低。这些数据表明，组织中CDC的稳态网络不足以免疫，并揭示了趋化因子驱动的肺CDC数量扩展的机制，从而放大了针对呼吸道病毒的T细胞反应。

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《Science Immunology》 |2021年第65期|Recruitment of dendritic/1-Recruitment of dendritic/15|共15页
作者
MAR CABEZA-CABRERIZO; CARLOS M. MINUTTI; MARIANA PEREIRA DA COSTA;
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Immunobiology Laboratory, Francis Crick Institute, 1 Midland Road, London NW1 1AT, UK;

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正文语种英语
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关键词
Influenzavirus A; Immunity; InfectionRecruitmentDendritic CellsprecursorsStem CellsT-LymphocytesRespirovirusChemokinesCCR2 ReceptorsVirus Diseases;

机译：流感病毒A;免疫;感染源性细胞培养系统细胞 - 淋巴细胞呼吸病毒病毒CCR2受体病毒病毒疾病;

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Recruitment of dendritic cell progenitors to foci of influenza A virus infection sustains immunity

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