| Literature DB >> 30799229 |
Ayako Shigeta1, Vincent Huang1, Jonathan Zuo1, Rana Besada1, Yasuhiro Nakashima1, Yan Lu2, Yichen Ding2, Matteo Pellegrini3, Rajan P Kulkarni4, Tzung Hsiai2, Arjun Deb5, Bin Zhou6, Haruko Nakano1, Atsushi Nakano7.
Abstract
During mammalian embryogenesis, de novo hematopoiesis occurs transiently in multiple anatomical sites including the yolk sac, dorsal aorta, and heart tube. A long-unanswered question is whether these local transient hematopoietic mechanisms are essential for embryonic growth. Here, we show that endocardial hematopoiesis is critical for cardiac valve remodeling as a source of tissue macrophages. Colony formation assay from explanted heart tubes and genetic lineage tracing with the endocardial specific Nfatc1-Cre mouse revealed that hemogenic endocardium is a de novo source of tissue macrophages in the endocardial cushion, the primordium of the cardiac valves. Surface marker characterization, gene expression profiling, and ex vivo phagocytosis assay revealed that the endocardially derived cardiac tissue macrophages play a phagocytic and antigen presenting role. Indeed, genetic ablation of endocardially derived macrophages caused severe valve malformation. Together, these data suggest that transient hemogenic activity in the endocardium is indispensable for the valvular tissue remodeling in the heart.Entities:
Keywords: cardiac tissue macrophage; cardiogenesis; congenital heart disease; hematopoiesis; hemogenic endocardium; multipotent cardiac progenitor cells; tissue macrophages; valve disease; valve remodeling; valvulogenesis
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Year: 2019 PMID: 30799229 PMCID: PMC6440481 DOI: 10.1016/j.devcel.2019.01.021
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 13.417