生物
合子
体细胞
生殖系
胚胎干细胞
谱系(遗传)
索马
进化生物学
祖细胞
遗传学
发育生物学
干细胞
系统发育学
胚胎发生
胚胎
基因
神经科学
作者
Tim H. H. Coorens,Luiza Moore,Philip S. Robinson,Rashesh Sanghvi,Joseph Christopher,James Hewinson,Moritz J. Przybilla,Andrew Lawson,Michael Spencer Chapman,Alex Cagan,Thomas R. W. Oliver,Matthew D. C. Neville,Yvette Hooks,Ayesha Noorani,Thomas J. Mitchell,Rebecca C. Fitzgerald,Peter J. Campbell,Iñigo Martincorena,Raheleh Rahbari,Michael R. Stratton
出处
期刊:Nature
[Springer Nature]
日期:2021-08-25
卷期号:597 (7876): 387-392
被引量:123
标识
DOI:10.1038/s41586-021-03790-y
摘要
Starting from the zygote, all cells in the human body continuously acquire mutations. Mutations shared between different cells imply a common progenitor and are thus naturally occurring markers for lineage tracing1,2. Here we reconstruct extensive phylogenies of normal tissues from three adult individuals using whole-genome sequencing of 511 laser capture microdissections. Reconstructed embryonic progenitors in the same generation of a phylogeny often contribute to different extents to the adult body. The degree of this asymmetry varies between individuals, with ratios between the two reconstructed daughter cells of the zygote ranging from 60:40 to 93:7. Asymmetries pervade subsequent generations and can differ between tissues in the same individual. The phylogenies resolve the spatial embryonic patterning of tissues, revealing contiguous patches of, on average, 301 crypts in the adult colonic epithelium derived from a most recent embryonic cell and also a spatial effect in brain development. Using data from ten additional men, we investigated the developmental split between soma and germline, with results suggesting an extraembryonic contribution to primordial germ cells. This research demonstrates that, despite reaching the same ultimate tissue patterns, early bottlenecks and lineage commitments lead to substantial variation in embryonic patterns both within and between individuals. Somatic mutations obtained from laser microdissected biopsies of human tissues are used to reconstruct the developmental phylogenies of these tissues back to the zygote.
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