Abstract

Chromatin was first defined by Flemming in 1882 as the `substance in the cell nucleus which is readily stained'that `is refractile to digestion'. The term stuck, and now is taken to refer to DNA (the readily stained component) and the associated proteins that make it refractile to digestion. It has become clear over the past twenty years that chromatin structure is vastly more dynamic than previously suspected. Regulation of chromatin structure frequently regulates the ability of proteins to access DNA, and in this manner plays a key role in regulating transcription, replication and recombination of the genome. The basic structural component of chromatin, the nucleosome, plays a central role in this regulation. The position of nucleosomes on the DNA can be changed, nucleosomes can be evicted, and nucleosomes can contain various histone variants and can be covalently modified in different ways, allowing them to have differential abilities to interact with the regulatory machinery. The dynamic nature of chromatin has been intensively studied for the past fifteen years, with much of the resultant information pertaining to the type and extent of covalent modification of the nucleosome. Information on the location of nucleosomes and on the full spectrum of proteins that might be involved in regulating a specific genomic locus has lagged behind this flood of information on covalent alterations to chromatin. The purpose of the experiments described in this application is to investigate how the location of nucleosomes can be altered in vitro and in vivo and to determine the full spectrum of proteins that might be involved in these types of regulation on a given genomic locus.
Three Aims are proposed:
Aim 1 will characterize nucleosome remodeling in vitro by examining individual remodeled products and through structural approaches;
Aim 2 will characterize structural changes to chromatin during regulation of a set of genes in cultured human cells;
and Aim 3 will develop technology to catalog proteins and RNA that bind to specific loci. Public Health Relevance: Epigenetic mechanisms impact the expression of the human genome by altering the ability of individual genes to be expressed in different cell types, and are known to contribute strongly to normal development and to many disease processes including cancer. These mechanisms rely in large part upon mechanisms to modify chromatin structure, the focus of this grant application. This application proposes experiments to understand how human chromatin structure might be regulated to effect changes in gene expression and as such is directly relevant to an understanding of numerous disease processes from cancer to infectious disease.

Public Health Relevance

Epigenetic mechanisms impact the expression of the human genome by altering the ability of individual genes to be expressed in different cell types, and are known to contribute strongly to normal development and to many disease processes including cancer. These mechanisms rely in large part upon mechanisms to modify chromatin structure, the focus of this grant application. This application proposes experiments to understand how human chromatin structure might be regulated to effect changes in gene expression and as such is directly relevant to an understanding of numerous disease processes from cancer to infectious disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37GM048405-19
Application #
8019037
Study Section
Nuclear Dynamics and Transport (NDT)
Program Officer
Carter, Anthony D
Project Start
1993-01-01
Project End
2013-12-31
Budget Start
2011-01-01
Budget End
2011-12-31
Support Year
19
Fiscal Year
2011
Total Cost
$394,662
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
073130411
City
Boston
State
MA
Country
United States
Zip Code
02199

  Publications

Ardehali, M Behfar; Anselmo, Anthony; Cochrane, Jesse C et al. (2017) Polycomb Repressive Complex 2 Methylates Elongin A to Regulate Transcription. Mol Cell 68:872-884.e6
Jaensch, Elizabeth S; Kundu, Sharmistha; Kingston, Robert E (2017) Multitasking by Polycomb response elements. Genes Dev 31:1069-1072
Mueller, Britta; Mieczkowski, Jakub; Kundu, Sharmistha et al. (2017) Widespread changes in nucleosome accessibility without changes in nucleosome occupancy during a rapid transcriptional induction. Genes Dev 31:451-462
Ray, Mridula K; Wiskow, Ole; King, Matthew J et al. (2016) CAT7 and cat7l Long Non-coding RNAs Tune Polycomb Repressive Complex 1 Function during Human and Zebrafish Development. J Biol Chem 291:19558-72
West, Jason A; Mito, Mari; Kurosaka, Satoshi et al. (2016) Structural, super-resolution microscopy analysis of paraspeckle nuclear body organization. J Cell Biol 214:817-30
Pulivarthy, Sandhya R; Lion, Mattia; Kuzu, Guray et al. (2016) Regulated large-scale nucleosome density patterns and precise nucleosome positioning correlate with V(D)J recombination. Proc Natl Acad Sci U S A 113:E6427-E6436
Yildirim, Ozlem; Kingston, Robert E (2016) Molecular Dissection of Chromatin Maturation via Click Chemistry. Curr Protoc Mol Biol 114:21.33.1-21.33.11
Schorderet, Patrick (2016) NEAT: a framework for building fully automated NGS pipelines and analyses. BMC Bioinformatics 17:53
Mieczkowski, Jakub; Cook, April; Bowman, Sarah K et al. (2016) MNase titration reveals differences between nucleosome occupancy and chromatin accessibility. Nat Commun 7:11485
Cajigas, Ivelisse; Leib, David E; Cochrane, Jesse et al. (2015) Evf2 lncRNA/BRG1/DLX1 interactions reveal RNA-dependent inhibition of chromatin remodeling. Development 142:2641-52

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