| Literature DB >> 27088311 |
Wenjuan Zhang1, Yaping Li1, Michael Kulik1, Rochelle L Tiedemann2, Keith D Robertson2, Stephen Dalton1, Shaying Zhao1.
Abstract
Nucleosomes are the basic unit of chromatin. Nucleosome positioning (NP) plays a key role in transcriptional regulation and other biological processes. To better understand NP we used MNase-seq to investigate changes that occur as human embryonic stem cells (hESCs) transition to nascent mesoderm and then to smooth muscle cells (SMCs). Compared to differentiated cell derivatives, nucleosome occupancy at promoters and other notable genic sites, such as exon/intron junctions and adjacent regions, in hESCs shows a stronger correlation with transcript abundance and is less influenced by sequence content. Upon hESC differentiation, genes being silenced, but not genes being activated, display a substantial change in nucleosome occupancy at their promoters. Genome-wide, we detected a shift of NP to regions of higher G+C content as hESCs differentiate to SMCs. Notably, genomic regions with higher nucleosome occupancy harbor twice as many G↔C changes but fewer than half A↔T changes, compared to regions with lower nucleosome occupancy. Finally, our analysis indicates that the hESC genome is not rearranged and has a sequence mutation rate resembling normal human genomes. Our study reveals another unique feature of hESC chromatin, and sheds light on the relationship between nucleosome occupancy and sequence G+C content.Entities:
Keywords: G+C content; MNase-seq; hESC differentiation; nucleosome occupancy; nucleosome positioning; sequence mutation; transcription
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Year: 2016 PMID: 27088311 PMCID: PMC4939925 DOI: 10.1080/15592294.2016.1176649
Source DB: PubMed Journal: Epigenetics ISSN: 1559-2294 Impact factor: 4.528