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首页> 外文期刊>Nature Communications >Non-classical tissue monocytes and two functionally distinct populations of interstitial macrophages populate the mouse lung
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Non-classical tissue monocytes and two functionally distinct populations of interstitial macrophages populate the mouse lung

机译:非古典组织单核细胞和两个功能性不同的间质巨噬细胞群填充了小鼠肺部

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摘要

Resident tissue macrophages (RTM) can fulfill various tasks during development, homeostasis, inflammation and repair. In the lung, non-alveolar RTM, called interstitial macrophages (IM), importantly contribute to tissue homeostasis but remain little characterized. Here we show, using single-cell RNA-sequencing (scRNA-seq), two phenotypically distinct subpopulations of long-lived monocyte-derived IM, i.e. CD206sup+/sup and CD206sup-/supIM, as well as a discrete population of extravasating CD64sup+/supCD16.2sup+/sup monocytes. CD206sup+/sup IM are peribronchial self-maintaining RTM that constitutively produce high levels of chemokines and immunosuppressive cytokines. Conversely, CD206sup-/supIM preferentially populate the alveolar interstitium and exhibit features of antigen-presenting cells. In addition, our data support that CD64sup+/supCD16.2sup+/sup monocytes arise from intravascular Ly-6Csuplo/sup patrolling monocytes that enter the tissue at steady-state to become putative precursors of CD206sup-/supIM. This study expands our knowledge about the complexity of lung IM and reveals an ontogenic pathway for one IM subset, an important step for elaborating future macrophage-targeted therapies.
机译:常住组织巨噬细胞(RTM)可以在开发,稳态,炎症和修复过程中满足各种任务。在肺中,非肺泡RTM称为间质巨噬细胞(IM),重要的是有助于组织稳态,但仍然很少表征。在这里,我们展示了使用单细胞RNA测序(ScRNA-SEQ),两种表型不同的长寿命的单核细胞衍生IM,即CD206 + 和CD206 - IM,以及离散群体外渗透CD64 + / sup> cd16.2 + 单核细胞。 CD206 + Im是泛血管连接的自我保持RTM,其构成趋于高水平的趋化因子和免疫抑制细胞因子。相反,CD206 - Im优先填充肺泡间质并表现出抗原呈递细胞的特征。此外,我们的数据支持该CD64 + cd16.2 + 单核细胞从血管内的ly-6c lo 巡逻单核细胞中出现,所述单核细胞在稳定上进入组织 - 成为CD206 - im的推定前体。本研究扩展了我们对肺部肺部复杂性的知识,并揭示了一个IM子集的肿瘤途径,这是制定未来巨噬细胞靶向疗法的重要步骤。

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