| Literature DB >> 33981037 |
Michael Spencer Chapman1,2,3, Anna Maria Ranzoni1,4,5, Brynelle Myers1,4,5, Nicholas Williams1, Tim H H Coorens1, Emily Mitchell1,3,4, Timothy Butler1, Kevin J Dawson1, Yvette Hooks1, Luiza Moore1,6, Jyoti Nangalia1,4,5, Philip S Robinson1,7, Kenichi Yoshida1, Elizabeth Hook6, Peter J Campbell8,9, Ana Cvejic10,11,12.
Abstract
The ontogeny of the human haematopoietic system during fetal development has previously been characterized mainly through careful microscopic observations1. Here we reconstruct a phylogenetic tree of blood development using whole-genome sequencing of 511 single-cell-derived haematopoietic colonies from healthy human fetuses at 8 and 18 weeks after conception, coupled with deep targeted sequencing of tissues of known embryonic origin. We found that, in healthy fetuses, individual haematopoietic progenitors acquire tens of somatic mutations by 18 weeks after conception. We used these mutations as barcodes and timed the divergence of embryonic and extra-embryonic tissues during development, and estimated the number of blood antecedents at different stages of embryonic development. Our data support a hypoblast origin of the extra-embryonic mesoderm and primitive blood in humans.Entities:
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Year: 2021 PMID: 33981037 DOI: 10.1038/s41586-021-03548-6
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962