Literature DB >> 21957152

Late-replicating heterochromatin is characterized by decreased cytosine methylation in the human genome.

Masako Suzuki1, Mayumi Oda, María-Paz Ramos, Marién Pascual, Kevin Lau, Edyta Stasiek, Frederick Agyiri, Reid F Thompson, Jacob L Glass, Qiang Jing, Richard Sandstrom, Melissa J Fazzari, R Scott Hansen, John A Stamatoyannopoulos, Andrew S McLellan, John M Greally.   

Abstract

Heterochromatin is believed to be associated with increased levels of cytosine methylation. With the recent availability of genome-wide, high-resolution molecular data reflecting chromatin organization and methylation, such relationships can be explored systematically. As well-defined surrogates for heterochromatin, we tested the relationship between DNA replication timing and DNase hypersensitivity with cytosine methylation in two human cell types, unexpectedly finding the later-replicating, more heterochromatic regions to be less methylated than early replicating regions. When we integrated gene-expression data into the study, we found that regions of increased gene expression were earlier replicating, as previously identified, and that transcription-targeted cytosine methylation in gene bodies contributes to the positive correlation with early replication. A self-organizing map (SOM) approach was able to identify genomic regions with early replication and increased methylation, but lacking annotated transcripts, loci missed in simple two variable analyses, possibly encoding unrecognized intergenic transcripts. We conclude that the relationship of cytosine methylation with heterochromatin is not simple and depends on whether the genomic context is tandemly repetitive sequences often found near centromeres, which are known to be heterochromatic and methylated, or the remaining majority of the genome, where cytosine methylation is targeted preferentially to the transcriptionally active, euchromatic compartment of the genome.

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Year:  2011        PMID: 21957152      PMCID: PMC3205568          DOI: 10.1101/gr.116509.110

Source DB:  PubMed          Journal:  Genome Res        ISSN: 1088-9051            Impact factor:   9.043


  42 in total

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3.  Overall DNA methylation and chromatin structure of normal and abnormal X chromosomes.

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4.  Inactive X chromosome has the highest concentration of unmethylated Hha I sites.

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5.  The DNMT3B DNA methyltransferase gene is mutated in the ICF immunodeficiency syndrome.

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6.  Satellite 2 methylation patterns in normal and ICF syndrome cells and association of hypomethylation with advanced replication.

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Review 7.  Evolution of chromosome bands: molecular ecology of noncoding DNA.

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Journal:  Nature       Date:  2007-06-14       Impact factor: 49.962

Review 9.  Forming facultative heterochromatin: silencing of an X chromosome in mammalian females.

Authors:  J C Chow; C J Brown
Journal:  Cell Mol Life Sci       Date:  2003-12       Impact factor: 9.261

10.  Genome-wide DNA replication profile for Drosophila melanogaster: a link between transcription and replication timing.

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Journal:  Nat Genet       Date:  2002-09-30       Impact factor: 38.330

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3.  Systematic determination of replication activity type highlights interconnections between replication, chromatin structure and nuclear localization.

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5.  The mutational landscape of human somatic and germline cells.

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6.  Kidney cancer is characterized by aberrant methylation of tissue-specific enhancers that are prognostic for overall survival.

Authors:  Caroline Y Hu; Davoud Mohtat; Yiting Yu; Yi-An Ko; Niraj Shenoy; Sanchari Bhattacharya; Maria C Izquierdo; Ae Seo Deok Park; Orsolya Giricz; Nishanth Vallumsetla; Krishna Gundabolu; Kristin Ware; Tushar D Bhagat; Masako Suzuki; James Pullman; X Shirley Liu; John M Greally; Katalin Susztak; Amit Verma
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Review 7.  DNA methylation signatures for breast cancer classification and prognosis.

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8.  DNA demethylation by 5-aza-2'-deoxycytidine is imprinted, targeted to euchromatin, and has limited transcriptional consequences.

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Review 9.  Genome-wide assays that identify and quantify modified cytosines in human disease studies.

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