Abstract

The three-dimensional organization of the genome is critical for regulation of gene expression, maintenance of genome stability and chromosome inheritance. Over the last several years there has been a tremendous increase in our knowledge of the spatial arrangements of chromosomes, and this is leading to insights into the molecular mechanisms that regulate genes, and how defects in genome folding can lead to human disease. We have developed powerful molecular and genomic technologies based on chromosome conformation capture (3C, 5C, Hi-C) to probe the three-dimensional structure of chromosomes. As cells go through the cell division cycle chromosomes alternate between two entirely different spatial conformations. We and others have used 3C-based assays to determine the structure of the human genome in interphase and in metaphase. In interphase the genome is composed of several different types of chromosomal domains, while within these domains genes are regulated by specific looping interactions between genes and their regulatory elements. A different structure is observed in mitotic cells, when chromosomes become highly compacted. We discovered that in mitosis chromosomes fold as linear arrays of consecutive chromatin loops. We have delineated a series of folding intermediates that show how the interphase conformation is converted into the metaphase state. These intermediates include extended linear loop arrays in prophase and more compacted helical arrays of nested loops in prometaphase. These studies lead to important new questions that we aim to address. First, it is not known in genomic detail how during prophase the interphase state is erased, chromosomes form initial loop arrays and sister chromatids become separated. Second, very little is known about the molecular machines that fold chromosomes. We propose innovative new strategies to identify new components of these machines that act during mitosis and interphase. Third, we hypothesize that these machines act through specific cis-elements that determine how and where they get loaded onto chromosomes, move to new sites and accumulate at yet other sites. We will identify and characterize these DNA elements that encode how the genome folds. Our proposed studies will uncover how the genome folds, unfolds and refolds.

Public Health Relevance

The human genome encodes the information required for normal human development. How the genome folds in three dimensions is now known to be critical for genome function, and defects in this folding can lead to human diseases such as cancer and developmental disorders. This proposal aims to unravel the mechanisms, proteins and DNA elements used by cells to modulate the 3D folding of their genomes during the cell cycle to ensure appropriate expression of their genes and accurate segregation of their chromosomes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Human Genome Research Institute (NHGRI)
Type
Research Project (R01)
Project #
2R01HG003143-14
Application #
9615577
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Pazin, Michael J
Project Start
2003-09-30
Project End
2022-05-31
Budget Start
2018-08-01
Budget End
2019-05-31
Support Year
14
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
University of Massachusetts Medical School Worcester
Department
Genetics
Type
Schools of Medicine
DUNS #
603847393
City
Worcester
State
MA
Country
United States
Zip Code

  Publications

Metkar, Mihir; Ozadam, Hakan; Lajoie, Bryan R et al. (2018) Higher-Order Organization Principles of Pre-translational mRNPs. Mol Cell 72:715-726.e3
Dixon, Jesse R; Xu, Jie; Dileep, Vishnu et al. (2018) Integrative detection and analysis of structural variation in cancer genomes. Nat Genet 50:1388-1398
Kundu, Sharmistha; Ji, Fei; Sunwoo, Hongjae et al. (2018) Polycomb Repressive Complex 1 Generates Discrete Compacted Domains that Change during Differentiation. Mol Cell 71:191
Oudelaar, A Marieke; Davies, James O J; Hanssen, Lars L P et al. (2018) Single-allele chromatin interactions identify regulatory hubs in dynamic compartmentalized domains. Nat Genet 50:1744-1751
Gibcus, Johan H; Samejima, Kumiko; Goloborodko, Anton et al. (2018) A pathway for mitotic chromosome formation. Science 359:
Rodríguez-Carballo, Eddie; Lopez-Delisle, Lucille; Zhan, Ye et al. (2017) The HoxD cluster is a dynamic and resilient TAD boundary controlling the segregation of antagonistic regulatory landscapes. Genes Dev 31:2264-2281
Belaghzal, Houda; Dekker, Job; Gibcus, Johan H (2017) Hi-C 2.0: An optimized Hi-C procedure for high-resolution genome-wide mapping of chromosome conformation. Methods 123:56-65
Oomen, Marlies E; Dekker, Job (2017) Epigenetic characteristics of the mitotic chromosome in 1D and 3D. Crit Rev Biochem Mol Biol 52:185-204
Nora, Elphège P; Goloborodko, Anton; Valton, Anne-Laure et al. (2017) Targeted Degradation of CTCF Decouples Local Insulation of Chromosome Domains from Genomic Compartmentalization. Cell 169:930-944.e22
Schalbetter, Stephanie Andrea; Goloborodko, Anton; Fudenberg, Geoffrey et al. (2017) SMC complexes differentially compact mitotic chromosomes according to genomic context. Nat Cell Biol 19:1071-1080

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