| Literature DB >> 27149841 |
Sarah Moyon1, Jimmy L Huynh2, Dipankar Dutta3, Fan Zhang1, Dan Ma4, Seungyeul Yoo5, Rebecca Lawrence1, Michael Wegner6, Gareth R John7, Ben Emery8, Catherine Lubetzki9, Robin J M Franklin4, Guoping Fan10, Jun Zhu5, Jeffrey L Dupree11, Patrizia Casaccia12.
Abstract
Oligodendrocytes derive from progenitors (OPCs) through the interplay of epigenomic and transcriptional events. By integrating high-resolution methylomics, RNA-sequencing, and multiple transgenic lines, this study defines the role of DNMT1 in developmental myelination. We detected hypermethylation of genes related to cell cycle and neurogenesis during differentiation of OPCs, yet genetic ablation of Dnmt1 resulted in inefficient OPC expansion and severe hypomyelination associated with ataxia and tremors in mice. This phenotype was not caused by lineage switch or massive apoptosis but was characterized by a profound defect of differentiation associated with changes in exon-skipping and intron-retention splicing events and by the activation of an endoplasmic reticulum stress response. Therefore, loss of Dnmt1 in OPCs is not sufficient to induce a lineage switch but acts as an important determinant of the coordination between RNA splicing and protein synthesis necessary for myelin formation.Entities:
Year: 2016 PMID: 27149841 PMCID: PMC5063656 DOI: 10.1016/j.celrep.2016.03.060
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423