Literature DB >> 26590169

Large-Scale Chromatin Structure-Function Relationships during the Cell Cycle and Development: Insights from Replication Timing.

Vishnu Dileep1, Juan Carlos Rivera-Mulia1, Jiao Sima1, David M Gilbert2.   

Abstract

Chromosome architecture has received a lot of attention since the recent development of genome-scale methods to measure chromatin interactions (Hi-C), enabling the first sequence-based models of chromosome tertiary structure. A view has emerged of chromosomes as a string of structural units (topologically associating domains; TADs) whose boundaries persist through the cell cycle and development. TADs with similar chromatin states tend to aggregate, forming spatially segregated chromatin compartments. However, high-resolution Hi-C has revealed substructure within TADs (subTADs) that poses a challenge for models that attribute significance to structural units at any given scale. More than 20 years ago, the DNA replication field independently identified stable structural (and functional) units of chromosomes (replication foci) as well as spatially segregated chromatin compartments (early and late foci), but lacked the means to link these units to genomic map units. Genome-wide studies of replication timing (RT) have now merged these two disciplines by identifying individual units of replication regulation (replication domains; RDs) that correspond to TADs and are arranged in 3D to form spatiotemporally segregated subnuclear compartments. Furthermore, classifying RDs/TADs by their constitutive versus developmentally regulated RT has revealed distinct classes of chromatin organization, providing unexpected insight into the relationship between large-scale chromosome structure and function.
Copyright © 2015 Cold Spring Harbor Laboratory Press; all rights reserved.

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Year:  2015        PMID: 26590169     DOI: 10.1101/sqb.2015.80.027284

Source DB:  PubMed          Journal:  Cold Spring Harb Symp Quant Biol        ISSN: 0091-7451


  35 in total

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4.  Spatio-temporal re-organization of replication foci accompanies replication domain consolidation during human pluripotent stem cell lineage specification.

Authors:  Korey A Wilson; Andrew G Elefanty; Edouard G Stanley; David M Gilbert
Journal:  Cell Cycle       Date:  2016-07-19       Impact factor: 4.534

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7.  Genome-wide analysis of replication timing by next-generation sequencing with E/L Repli-seq.

Authors:  Claire Marchal; Takayo Sasaki; Daniel Vera; Korey Wilson; Jiao Sima; Juan Carlos Rivera-Mulia; Claudia Trevilla-García; Coralin Nogues; Ebtesam Nafie; David M Gilbert
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8.  Bacterial artificial chromosomes establish replication timing and sub-nuclear compartment de novo as extra-chromosomal vectors.

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9.  Cross-talk between Lysine-Modifying Enzymes Controls Site-Specific DNA Amplifications.

Authors:  Sweta Mishra; Capucine Van Rechem; Sangita Pal; Thomas L Clarke; Damayanti Chakraborty; Sarah D Mahan; Joshua C Black; Sedona E Murphy; Michael S Lawrence; Danette L Daniels; Johnathan R Whetstine
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10.  Stability of patient-specific features of altered DNA replication timing in xenografts of primary human acute lymphoblastic leukemia.

Authors:  Takayo Sasaki; Juan Carlos Rivera-Mulia; Daniel Vera; Jared Zimmerman; Sunny Das; Michelle Padget; Naoto Nakamichi; Bill H Chang; Jeff Tyner; Brian J Druker; Andrew P Weng; Curt I Civin; Connie J Eaves; David M Gilbert
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