IL-12介导T-bet表达的髓样细胞依赖宿主对弓形虫的抵抗力

Q3 Medicine
Madison L Schanz, Abigail M Bitters, Kamryn E Zadeii, Dana Joulani, Angela K Chamberlain, Américo H López-Yglesias
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引用次数: 0

摘要

为了抵御弓形虫等细胞内病原体,宿主会产生强大的 1 型免疫反应。具体来说,宿主对弓形虫的防御是由 IL-12 依赖性 IFN-γ 反应决定的,这种反应对宿主的抵抗力至关重要。此前,我们证明宿主的抵抗力是由 T-bet 依赖性 ILC 衍生的 IFN-γ 通过在寄生虫感染期间维持 IRF8+常规 1 型树突状细胞而介导的。因此,我们假设先天性淋巴细胞对宿主的生存是不可或缺的。令人惊讶的是,我们观察到,T-bet 缺失的小鼠比淋巴细胞缺乏的小鼠更快被感染,这表明存在一种未知的依赖于 T-bet 的宿主防御途径。对寄生虫介导的炎症性髓系细胞的分析发现了一个新的亚群--T-bet+髓系细胞(TMCs)。我们的研究结果表明,与其他专业吞噬细胞相比,TMCs 的细胞内寄生虫负荷最大,这表明它们与主动杀灭淋球菌有关。从机理上讲,我们确定了 IL-12 是感染期间诱导炎性 TMCs 的必要条件,而且这些细胞与宿主的存活有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
IL-12 Mediates T-bet-Expressing Myeloid Cell-Dependent Host Resistance against Toxoplasma gondii.

To defend against intracellular pathogens such as Toxoplasma gondii, the host generates a robust type 1 immune response. Specifically, host defense against T. gondii is defined by an IL-12-dependent IFN-γ response that is critical for host resistance. Previously, we demonstrated that host resistance is mediated by T-bet-dependent ILC-derived IFN-γ by maintaining IRF8+ conventional type 1 dendritic cells during parasitic infection. Therefore, we hypothesized that innate lymphoid cells are indispensable for host survival. Surprisingly, we observed that T-bet-deficient mice succumb to infection quicker than do mice lacking lymphocytes, suggesting an unknown T-bet-dependent-mediated host defense pathway. Analysis of parasite-mediated inflammatory myeloid cells revealed a novel subpopulation of T-bet+ myeloid cells (TMCs). Our results reveal that TMCs have the largest intracellular parasite burden compared with other professional phagocytes, suggesting they are associated with active killing of T. gondii. Mechanistically, we established that IL-12 is necessary for the induction of inflammatory TMCs during infection and these cells are linked to a role in host survival.

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来源期刊
CiteScore
3.70
自引率
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