| Literature DB >> 35482005 |
Kuo Liu1,2,3, Hengwei Jin2, Muxue Tang2, Shaohua Zhang2, Xueying Tian4, Mingjun Zhang2, Ximeng Han2,3, Xiuxiu Liu2, Juan Tang2, Wenjuan Pu2, Yan Li2, Lingjuan He5, Zhongzhou Yang6, Kathy O Lui7, Bin Zhou1,2,4,3.
Abstract
Tissue-resident macrophages play essential functions in the maintenance of tissue homeostasis and repair. Recently, the endocardium has been reported as a de novo hemogenic site for the contribution of hematopoietic cells, including cardiac macrophages, during embryogenesis. These observations challenge the current consensus that hematopoiesis originates from the hemogenic endothelium within the yolk sac and dorsal aorta. Whether the developing endocardium has such a hemogenic potential requires further investigation. Here, we generated new genetic tools to trace endocardial cells and reassessed their potential contribution to hematopoietic cells in the developing heart. Fate-mapping analyses revealed that the endocardium contributed minimally to cardiac macrophages and circulating blood cells. Instead, cardiac macrophages were mainly derived from the endothelium during primitive/transient definitive (yolk sac) and definitive (dorsal aorta) hematopoiesis. Our findings refute the concept of endocardial hematopoiesis, suggesting that the developing endocardium gives rise minimally to hematopoietic cells, including cardiac macrophages.Entities:
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Year: 2022 PMID: 35482005 PMCID: PMC9059379 DOI: 10.1083/jcb.202108093
Source DB: PubMed Journal: J Cell Biol ISSN: 0021-9525 Impact factor: 8.077