| Literature DB >> 29551301 |
Michael J Ziller1, Juan A Ortega2, Katharina A Quinlan3, David P Santos2, Hongcang Gu4, Eric J Martin2, Christina Galonska5, Ramona Pop6, Susanne Maidl1, Alba Di Pardo2, Mei Huang7, Herbert Y Meltzer8, Andreas Gnirke4, C J Heckman9, Alexander Meissner10, Evangelos Kiskinis11.
Abstract
The somatic DNA methylation (DNAme) landscape is established early in development but remains highly dynamic within focal regions that overlap with gene regulatory elements. The significance of these dynamic changes, particularly in the central nervous system, remains unresolved. Here, we utilize a powerful human embryonic stem cell differentiation model for the generation of motor neurons (MNs) in combination with genetic mutations in the de novo DNAme machinery. We quantitatively dissect the role of DNAme in directing somatic cell fate with high-resolution genome-wide bisulfite-, bulk-, and single-cell-RNA sequencing. We find defects in neuralization and MN differentiation in DNMT3A knockouts (KO) that can be rescued by the targeting of DNAme to key developmental loci using catalytically inactive dCas9. We also find decreased dendritic arborization and altered electrophysiological properties in DNMT3A KO MNs. Our work provides a list of DNMT3A-regulated targets and a mechanistic link between de novo DNAme, cellular differentiation, and human MN function.Entities:
Keywords: DNA methylation; DNMT3A; ESCs; cell fate; epigenetics; motor neurons; neurogenesis; spinal cord development
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Year: 2018 PMID: 29551301 PMCID: PMC6535433 DOI: 10.1016/j.stem.2018.02.012
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633