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CD127 印记赋予功能性异质性,从而使炎症性疾病中的单核细胞反应多样化。

CD127 imprints functional heterogeneity to diversify monocyte responses in inflammatory diseases.

机构信息

Institute for Immunology and School of Medicine, Tsinghua University, Beijing, China.

Beijing Key Laboratory for Immunological Research on Chronic Diseases, Beijing, China.

出版信息

J Exp Med. 2022 Feb 7;219(2). doi: 10.1084/jem.20211191. Epub 2022 Jan 11.

Abstract

Inflammatory monocytes are key mediators of acute and chronic inflammation; yet, their functional diversity remains obscure. Single-cell transcriptome analyses of human inflammatory monocytes from COVID-19 and rheumatoid arthritis patients revealed a subset of cells positive for CD127, an IL-7 receptor subunit, and such positivity rendered otherwise inert monocytes responsive to IL-7. Active IL-7 signaling engaged epigenetically coupled, STAT5-coordinated transcriptional programs to restrain inflammatory gene expression, resulting in inverse correlation between CD127 expression and inflammatory phenotypes in a seemingly homogeneous monocyte population. In COVID-19 and rheumatoid arthritis, CD127 marked a subset of monocytes/macrophages that retained hypoinflammatory phenotypes within the highly inflammatory tissue environments. Furthermore, generation of an integrated expression atlas revealed unified features of human inflammatory monocytes across different diseases and different tissues, exemplified by those of the CD127high subset. Overall, we phenotypically and molecularly characterized CD127-imprinted functional heterogeneity of human inflammatory monocytes with direct relevance for inflammatory diseases.

摘要

炎性单核细胞是急性和慢性炎症的关键介质;然而,它们的功能多样性仍然不清楚。对来自 COVID-19 和类风湿关节炎患者的人炎性单核细胞的单细胞转录组分析显示,一小部分细胞对 CD127(IL-7 受体亚基)呈阳性,这种阳性使原本不活跃的单核细胞对 IL-7 有反应。活性 IL-7 信号通过表观遗传耦联、STAT5 协调的转录程序来抑制炎症基因表达,导致在看似同质的单核细胞群体中,CD127 表达与炎症表型呈负相关。在 COVID-19 和类风湿关节炎中,CD127 标记了单核细胞/巨噬细胞的一个亚群,在高度炎症的组织环境中保留了低炎症表型。此外,综合表达图谱的生成揭示了不同疾病和不同组织中人类炎性单核细胞的统一特征,以 CD127high 亚群为例。总体而言,我们从表型和分子上对具有直接相关性的人类炎性单核细胞的 CD127 印迹功能异质性进行了特征描述炎症性疾病。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/464f/8757045/e7f521335c78/JEM_20211191_GA.jpg

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