Single-cell analysis of RORα tracer mouse lung reveals ILC progenitors and effector ILC2 subsets.

Maryam Ghaedi, Zi Yi Shen, Mona Orangi, Itziar Martinez-Gonzalez, Lisa Wei, Xiaoxiao Lu, Arundhoti Das, Alireza Heravi-Moussavi, Marco A Marra, Avinash Bhandoola, Fumio Takei
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Abstract

Lung group 2 innate lymphoid cells (ILC2s) drive allergic inflammation and promote tissue repair. ILC2 development is dependent on the transcription factor retinoic acid receptor-related orphan receptor (RORα), which is also expressed in common ILC progenitors. To elucidate the developmental pathways of lung ILC2s, we generated RORα lineage tracer mice and performed single-cell RNA sequencing, flow cytometry, and functional analyses. In adult mouse lungs, we found an IL-18Rα+ST2- population different from conventional IL-18Rα-ST2+ ILC2s. The former was GATA-3intTcf7EGFP+Kit+, produced few cytokines, and differentiated into multiple ILC lineages in vivo and in vitro. In neonatal mouse lungs, three ILC populations were identified, namely an ILC progenitor population similar to that in adult lungs and two distinct effector ILC2 subsets that differentially produced type 2 cytokines and amphiregulin. Lung ILC progenitors might actively contribute to ILC-poiesis in neonatal and inflamed adult lungs. In addition, neonatal lung ILC2s include distinct proinflammatory and tissue-repairing subsets.

RORα 示踪小鼠肺单细胞分析揭示了 ILC 祖细胞和效应 ILC2 亚群。
肺部第 2 组先天性淋巴细胞(ILC2)驱动过敏性炎症并促进组织修复。ILC2的发育依赖于转录因子视黄酸受体相关孤儿受体(RORα),它也表达于常见的ILC祖细胞。为了阐明肺ILC2的发育途径,我们产生了RORα系示踪小鼠,并进行了单细胞RNA测序、流式细胞术和功能分析。在成年小鼠肺中,我们发现了不同于传统 IL-18Rα-ST2+ ILC2 的 IL-18Rα+ST2 群体。前者为 GATA-3intTcf7EGFP+Kit+,很少产生细胞因子,并在体内和体外分化为多个 ILC 系。在新生小鼠肺部,发现了三种 ILC 群体,即与成人肺部类似的 ILC 祖细胞群体和两种不同的效应 ILC2 亚群,它们能不同程度地产生 2 型细胞因子和两性胰岛素。肺ILC祖细胞可能对新生儿和发炎的成人肺中的ILC-poiesis做出了积极贡献。此外,新生儿肺ILC2包括不同的促炎症亚群和组织修复亚群。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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