| Literature DB >> 30606806 |
Dario Nicetto1,2,3, Greg Donahue1,2,3, Tanya Jain1,2,3, Tao Peng4,5, Simone Sidoli2,6, Lihong Sheng2,3, Thomas Montavon7, Justin S Becker1,2,3, Jessica M Grindheim1,2,3, Kimberly Blahnik1,2,3, Benjamin A Garcia2,6, Kai Tan3,4,5,8, Roberto Bonasio2,3, Thomas Jenuwein7, Kenneth S Zaret9,2,3.
Abstract
Gene silencing by chromatin compaction is integral to establishing and maintaining cell fates. Trimethylated histone 3 lysine 9 (H3K9me3)-marked heterochromatin is reduced in embryonic stem cells compared to differentiated cells. However, the establishment and dynamics of closed regions of chromatin at protein-coding genes, in embryologic development, remain elusive. We developed an antibody-independent method to isolate and map compacted heterochromatin from low-cell number samples. We discovered high levels of compacted heterochromatin, H3K9me3-decorated, at protein-coding genes in early, uncommitted cells at the germ-layer stage, undergoing profound rearrangements and reduction upon differentiation, concomitant with cell type-specific gene expression. Perturbation of the three H3K9me3-related methyltransferases revealed a pivotal role for H3K9me3 heterochromatin during lineage commitment at the onset of organogenesis and for lineage fidelity maintenance.Entities:
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Year: 2019 PMID: 30606806 PMCID: PMC6664818 DOI: 10.1126/science.aau0583
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728