Chromatin in active regions of eukaryotic genomes undergoes extensive disruption and replacement of nucleosomes. New models suggest that nucleosome dynamics are critical to both increase DNA accessibility, to limit transcription factor binding, and to protect the genome from damage. The long-term goal of this project is to define the components involved in nucleosome dynamics and how these are important for genome function. Nucleosome replacement in all animals uses the conserved histone H3.3 variant, and the ATRX/Xnp chromatin remodeler has been implicated in H3.3 deposition into chromatin. We have developed methods to track H3.3 deposition in Drosophila, and model examples of nucleosome-depleted chromatin. In this proposal, we use these tools in combination with mutations in key factors to characterize the response of cells to chromatin gaps A second approach in this proposal uses a new method to visualize alternative occupancies of transcription factors and nucleosomes across the genome.
In Aim 1, we will define the importance of Drosophila ATRX/Xnp and associated factors for rebuilding nucleosomes at disrupted chromatin.
In Aim 2 we examine Polycomb Response Elements as natural examples of nucleosome-depleted chromatin. We analyze the role of ATRX/Xnp and other chromatin remodelers in driving cycles of nucleosome displacement and replacement. Finally, we determine the importance of nucleosome dynamics for factor binding in regulatory elements. These studies have broad relevance for understanding the integration of sequence-specific DNA-binding proteins, nucleosome remodeling, and intrinsic sequence features in dynamic chromatin regions.

Public Health Relevance

Eukaryotic genomes are packaged into chromatin, and replication, repair, and gene regulation require dynamic changes to access DNA. Our project will investigate the roles of nucleosome dynamics in integrating DNA- binding proteins, histone deposition, and nucleosome remodeling in transcribed genes and regulatory elements. These studies have implications for human diseases caused by chromatin defects, including cancer, neural dysfunction, and infertility.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
7R01GM098349-03
Application #
8889273
Study Section
Molecular Genetics A Study Section (MGA)
Program Officer
Carter, Anthony D
Project Start
2013-09-01
Project End
2017-06-30
Budget Start
2015-07-01
Budget End
2016-06-30
Support Year
3
Fiscal Year
2015
Total Cost
$343,200
Indirect Cost
$148,200
Name
Fred Hutchinson Cancer Research Center
Department
Type
DUNS #
078200995
City
Seattle
State
WA
Country
United States
Zip Code
98109
Kasinathan, Bhavatharini; Ahmad, Kami; Malik, Harmit S (2017) Waddington Redux: De Novo Mutations Underlie the Genetic Assimilation of Stress-Induced Phenocopies in Drosophila melanogaster. Genetics 207:49-51
Ramachandran, Srinivas; Ahmad, Kami; Henikoff, Steven (2017) Capitalizing on disaster: Establishing chromatin specificity behind the replication fork. Bioessays 39:
Orsi, Guillermo A; Kasinathan, Sivakanthan; Zentner, Gabriel E et al. (2015) Mapping regulatory factors by immunoprecipitation from native chromatin. Curr Protoc Mol Biol 110:21.31.1-25