| Literature DB >> 25139355 |
Laura Padrón-Barthe1, Susana Temiño1, Cristina Villa del Campo1, Laura Carramolino1, Joan Isern1, Miguel Torres1.
Abstract
The first blood and endothelial cells of amniote embryos appear in close association in the blood islands of the yolk sac (YS). This association and in vitro lineage analyses have suggested a common origin from mesodermal precursors called hemangioblasts, specified in the primitive streak during gastrulation. Fate mapping and chimera studies, however, failed to provide strong evidence for a common origin in the early mouse YS. Additional in vitro studies suggest instead that mesodermal precursors first generate hemogenic endothelium, which then generate blood cells in a linear sequence. We conducted an in vivo clonal analysis to determine the potential of individual cells in the mouse epiblast, primitive streak, and early YS. We found that early YS blood and endothelial lineages mostly derive from independent epiblast populations, specified before gastrulation. Additionally, a subpopulation of the YS endothelium has hemogenic activity and displays characteristics similar to those found later in the embryonic hemogenic endothelium. Our results show that the earliest blood and endothelial cell populations in the mouse embryo are specified independently, and that hemogenic endothelium first appears in the YS and produces blood precursors with markers related to definitive hematopoiesis.Entities:
Mesh:
Year: 2014 PMID: 25139355 PMCID: PMC4199954 DOI: 10.1182/blood-2013-12-545939
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113