Canonical nucleosome organization at promoters forms during genome activation
- Yong Zhang1,
- Nadine L Vastenhouw2,
- Jianxing Feng1,
- Kai Fu1,
- Chenfei Wang1,
- Ying Ge1,
- Paul van Hummelen3,
- Alexander F Schier2 and
- Xiaole Shirley Liu4,5
- 1 Tongji University;
- 2 Harvard University;
- 3 Dana-Farber Cancer Institute;
- 4 Dana-Farber Cancer Institute / Harvard School of Public Health
- ↵* Corresponding author; email: xsliu{at}jimmy.harvard.edu
Abstract
The organization of nucleosomes influences transcriptional activity by controlling accessibility of DNA binding proteins to the genome. Genome-wide nucleosome binding profiles have identified a canonical nucleosome organization at gene promoters, where arrays of well-positioned nucleosomes emanate from nucleosome-depleted regions. The mechanisms of formation and the function of canonical promoter nucleosome organization remain unclear. Here we analyze the genome-wide location of nucleosomes during zebrafish embryogenesis and show that well-positioned nucleosome arrays appear on thousands of promoters during the activation of the zygotic genome. The formation of canonical promoter nucleosome organization is independent of DNA sequence preference, transcriptional elongation, and robust RNA polymerase II (Pol II) binding. Instead, canonical promoter nucleosome organization correlates with the presence of Histone H3 Lysine 4 trimethylation (H3K4me3) and affects future transcriptional activation. These findings reveal that genome activation is central to the organization of nucleosome arrays during early embryogenesis.
- Received March 15, 2013.
- Accepted November 25, 2013.
- Published by Cold Spring Harbor Laboratory Press
This manuscript is Open Access.
This article, published in Genome Research, is available under a Creative Commons License (Attribution-NonCommercial 3.0 Unported), as described at http://creativecommons.org/licenses/by-nc/3.0/.
