Publication | Open Access
Different mutational rates and mechanisms in human cells at pregastrulation and neurogenesis
282
Citations
37
References
2017
Year
Clonal Cell PopulationsBrain DevelopmentGeneticsEpigeneticsEmbryologyHuman CellsNeurogenesisSomatic MosaicismNeurogeneticsGenome InstabilityMutation RateMorphogenesisEmbryonic DevelopmentCell BiologyDifferent Mutational RatesDevelopmental BiologySomatic VariantSomatic Cell GeneticsStem Cell ResearchHuman Embryonic DevelopmentCell Fate DeterminationMedicineNeural Stem CellCell Development
Somatic mosaicism in the human brain may alter function of individual neurons. We analyzed genomes of single cells from the forebrains of three human fetuses (15 to 21 weeks postconception) using clonal cell populations. We detected 200 to 400 single-nucleotide variations (SNVs) per cell. SNV patterns resembled those found in cancer cell genomes, indicating a role of background mutagenesis in cancer. SNVs with a frequency of >2% in brain were also present in the spleen, revealing a pregastrulation origin. We reconstructed cell lineages for the first five postzygotic cleavages and calculated a mutation rate of ~1.3 mutations per division per cell. Later in development, during neurogenesis, the mutation spectrum shifted toward oxidative damage, and the mutation rate increased. Both neurogenesis and early embryogenesis exhibit substantially more mutagenesis than adulthood.
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