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Literature DB >> 34001904

Genetic fate-mapping reveals surface accumulation but not deep organ invasion of pleural and peritoneal cavity macrophages following injury.

Hengwei Jin¹, Kuo Liu^1,2, Juan Tang¹, Xiuzhen Huang¹, Haixiao Wang¹, Qianyu Zhang³, Huan Zhu¹, Yan Li¹, Wenjuan Pu¹, Huan Zhao¹, Lingjuan He¹, Yi Li¹, Shaohua Zhang¹, Zhenqian Zhang¹, Yufei Zhao⁴, Yanqing Qin⁵, Stefan Pflanz⁶, Karim E I Kasmi⁶, Weiyi Zhang⁶, Zhaoyuan Liu⁷, Florent Ginhoux⁸, Yong Ji⁹, Ben He¹⁰, Lixin Wang⁴, Bin Zhou^11,12,13.

Abstract

During injury, monocytes are recruited from the circulation to inflamed tissues and differentiate locally into mature macrophages, with prior reports showing that cavity macrophages of the peritoneum and pericardium invade deeply into the respective organs to promote repair. Here we report a dual recombinase-mediated genetic system designed to trace cavity macrophages in vivo by intersectional detection of two characteristic markers. Lineage tracing with this method shows accumulation of cavity macrophages during lung and liver injury on the surface of visceral organs without penetration into the parenchyma. Additional data suggest that these peritoneal or pleural cavity macrophages do not contribute to tissue repair and regeneration. Our in vivo genetic targeting approach thus provides a reliable method to identify and characterize cavity macrophages during their development and in tissue repair and regeneration, and distinguishes these cells from other lineages.

Entities: CellLine Chemical Disease Gene Species

Year: 2021 PMID： 34001904 DOI： 10.1038/s41467-021-23197-7

Source DB: PubMed Journal: Nat Commun ISSN： 2041-1723 Impact factor: 14.919

62 in total

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9. A novel lineage of osteoprogenitor cells with dual epithelial and mesenchymal properties govern maxillofacial bone homeostasis and regeneration after MSFL.

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