Genome accessibility is widely preserved and locally modulated during mitosis
- Chris C-S Hsiung1,
- Christapher S Morrissey2,
- Maheshi Udugama1,
- Christopher L Frank3,
- Cheryl A Keller2,
- Songjoon Baek4,
- Belinda Giardine2,
- Gregory E Crawford3,
- Myong-Hee Sung4,
- Ross C Hardison2 and
- Gerd A Blobel1,5
- 1 The Children's Hospital of Philadelphia;
- 2 Pennsylvania State University;
- 3 Duke University;
- 4 National Cancer Institute
- ↵* Corresponding author; email: blobel{at}email.chop.edu
Abstract
Mitosis entails global alterations to chromosome structure and nuclear architecture, concomitant with transient silencing of transcription. How cells transmit transcriptional states through mitosis remains incompletely understood. While many nuclear factors dissociate from mitotic chromosomes, the observation that certain nuclear factors and chromatin features remain associated with individual loci during mitosis originated the hypothesis that such mitotically retained molecular signatures could provide transcriptional memory through mitosis. To understand the role of chromatin structure in mitotic memory, we obtained the first genome-wide view of chromatin accessibility in interphase and mitosis at two stages of cellular maturation in a murine erythroblast model. Despite chromosome condensation during mitosis visible by microscopy, the landscape of chromatin accessibility at the macromolecular level is largely unaltered. However, mitotic chromatin accessibility is locally dynamic, with individual loci maintaining none, some, or all of their interphase accessibility. Mitotic reduction in accessibility occurs primarily within narrow, highly DNase hypersensitive sites that frequently coincide with transcription factor binding sites, whereas broader domains of moderate accessibility tend to be more stable. In mitosis, proximal promoters generally maintain their accessibility more strongly, whereas distal regulatory elements tend to lose accessibility. Large domains of DNA hypomethylation mark a subset of promoters that retain accessibility during mitosis and across many cell types in interphase. Erythroid transcription factor GATA1 exerts site-specific changes in interphase accessibility that are most pronounced at distal regulatory elements, but has little influence on mitotic accessibility. We conclude that features of open chromatin are remarkably stable through mitosis, but are modulated at the level of individual genes and regulatory elements.
- Received June 28, 2014.
- Accepted November 3, 2014.
- Published by Cold Spring Harbor Laboratory Press
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