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Extensive phylogenies of human development inferred from somatic mutations

机译:从躯体突变推断人类发展的广泛系统发作

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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 tracing~(1,2). 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.
机译:从Zygote开始,人体中的所有细胞都不断获得突变。在不同细胞之间共享的突变意味着常见的祖细胞,因此是用于谱系追踪的天然存在的标记〜(1,2)。在这里,我们使用511激光捕获微散射的全基因组测序重建来自三个成年个体的正常组织的广泛文学系统。同样产生的体内发生的重建胚胎祖细胞通常有助于成人体的不同范围。这种不对称的程度在个体之间变化,比率之间的两个重建的子细胞之间的比率范围为60:40至93:7。不对称普遍的后代,同一个人的组织之间可以不同。系统发电机解析组织的空间胚胎图案化,揭示了衍生自最新胚胎细胞的成年结肠上皮中的连续斑块,以及脑发育中的空间效应。使用来自十个额外男性的数据,我们调查了Soma和Germline之间的发育分裂,结果表明对原始生殖细胞的特征贡献。这项研究表明,尽管达到了相同的终极组织模式,早期瓶颈和谱系承诺导致个人内部和之间的胚胎模式的大量变化。

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