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The IG-DMR and the MEG3-DMR at Human Chromosome 14q32.2: Hierarchical Interaction and Distinct Functional Properties as Imprinting Control Centers

Human chromosome 14q32.2 harbors the germline-derived primary DLK1-MEG3 intergenic differentially methylated region (IG-DMR) and the postfertilization-derived secondary MEG3-DMR, together with multiple imprinted genes. Although previous studies in cases with microdeletions and epimutations affecting...

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Autores principales: Kagami, Masayo, O'Sullivan, Maureen J., Green, Andrew J., Watabe, Yoshiyuki, Arisaka, Osamu, Masawa, Nobuhide, Matsuoka, Kentarou, Fukami, Maki, Matsubara, Keiko, Kato, Fumiko, Ferguson-Smith, Anne C., Ogata, Tsutomu
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2887472/
https://www.ncbi.nlm.nih.gov/pubmed/20585555
http://dx.doi.org/10.1371/journal.pgen.1000992
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author Kagami, Masayo
O'Sullivan, Maureen J.
Green, Andrew J.
Watabe, Yoshiyuki
Arisaka, Osamu
Masawa, Nobuhide
Matsuoka, Kentarou
Fukami, Maki
Matsubara, Keiko
Kato, Fumiko
Ferguson-Smith, Anne C.
Ogata, Tsutomu
author_facet Kagami, Masayo
O'Sullivan, Maureen J.
Green, Andrew J.
Watabe, Yoshiyuki
Arisaka, Osamu
Masawa, Nobuhide
Matsuoka, Kentarou
Fukami, Maki
Matsubara, Keiko
Kato, Fumiko
Ferguson-Smith, Anne C.
Ogata, Tsutomu
author_sort Kagami, Masayo
collection PubMed
description Human chromosome 14q32.2 harbors the germline-derived primary DLK1-MEG3 intergenic differentially methylated region (IG-DMR) and the postfertilization-derived secondary MEG3-DMR, together with multiple imprinted genes. Although previous studies in cases with microdeletions and epimutations affecting both DMRs and paternal/maternal uniparental disomy 14-like phenotypes argue for a critical regulatory function of the two DMRs for the 14q32.2 imprinted region, the precise role of the individual DMR remains to be clarified. We studied an infant with upd(14)pat body and placental phenotypes and a heterozygous microdeletion involving the IG-DMR alone (patient 1) and a neonate with upd(14)pat body, but no placental phenotype and a heterozygous microdeletion involving the MEG3-DMR alone (patient 2). The results generated from the analysis of these two patients imply that the IG-DMR and the MEG3-DMR function as imprinting control centers in the placenta and the body, respectively, with a hierarchical interaction for the methylation pattern in the body governed by the IG-DMR. To our knowledge, this is the first study demonstrating an essential long-range imprinting regulatory function for the secondary DMR.
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spelling pubmed-28874722010-06-22 The IG-DMR and the MEG3-DMR at Human Chromosome 14q32.2: Hierarchical Interaction and Distinct Functional Properties as Imprinting Control Centers Kagami, Masayo O'Sullivan, Maureen J. Green, Andrew J. Watabe, Yoshiyuki Arisaka, Osamu Masawa, Nobuhide Matsuoka, Kentarou Fukami, Maki Matsubara, Keiko Kato, Fumiko Ferguson-Smith, Anne C. Ogata, Tsutomu PLoS Genet Research Article Human chromosome 14q32.2 harbors the germline-derived primary DLK1-MEG3 intergenic differentially methylated region (IG-DMR) and the postfertilization-derived secondary MEG3-DMR, together with multiple imprinted genes. Although previous studies in cases with microdeletions and epimutations affecting both DMRs and paternal/maternal uniparental disomy 14-like phenotypes argue for a critical regulatory function of the two DMRs for the 14q32.2 imprinted region, the precise role of the individual DMR remains to be clarified. We studied an infant with upd(14)pat body and placental phenotypes and a heterozygous microdeletion involving the IG-DMR alone (patient 1) and a neonate with upd(14)pat body, but no placental phenotype and a heterozygous microdeletion involving the MEG3-DMR alone (patient 2). The results generated from the analysis of these two patients imply that the IG-DMR and the MEG3-DMR function as imprinting control centers in the placenta and the body, respectively, with a hierarchical interaction for the methylation pattern in the body governed by the IG-DMR. To our knowledge, this is the first study demonstrating an essential long-range imprinting regulatory function for the secondary DMR. Public Library of Science 2010-06-17 /pmc/articles/PMC2887472/ /pubmed/20585555 http://dx.doi.org/10.1371/journal.pgen.1000992 Text en Kagami et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Kagami, Masayo
O'Sullivan, Maureen J.
Green, Andrew J.
Watabe, Yoshiyuki
Arisaka, Osamu
Masawa, Nobuhide
Matsuoka, Kentarou
Fukami, Maki
Matsubara, Keiko
Kato, Fumiko
Ferguson-Smith, Anne C.
Ogata, Tsutomu
The IG-DMR and the MEG3-DMR at Human Chromosome 14q32.2: Hierarchical Interaction and Distinct Functional Properties as Imprinting Control Centers
title The IG-DMR and the MEG3-DMR at Human Chromosome 14q32.2: Hierarchical Interaction and Distinct Functional Properties as Imprinting Control Centers
title_full The IG-DMR and the MEG3-DMR at Human Chromosome 14q32.2: Hierarchical Interaction and Distinct Functional Properties as Imprinting Control Centers
title_fullStr The IG-DMR and the MEG3-DMR at Human Chromosome 14q32.2: Hierarchical Interaction and Distinct Functional Properties as Imprinting Control Centers
title_full_unstemmed The IG-DMR and the MEG3-DMR at Human Chromosome 14q32.2: Hierarchical Interaction and Distinct Functional Properties as Imprinting Control Centers
title_short The IG-DMR and the MEG3-DMR at Human Chromosome 14q32.2: Hierarchical Interaction and Distinct Functional Properties as Imprinting Control Centers
title_sort ig-dmr and the meg3-dmr at human chromosome 14q32.2: hierarchical interaction and distinct functional properties as imprinting control centers
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2887472/
https://www.ncbi.nlm.nih.gov/pubmed/20585555
http://dx.doi.org/10.1371/journal.pgen.1000992
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