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The Evolution of Mammalian Genomic Imprinting Was Accompanied by the Acquisition of Novel CpG Islands

Parent-of-origin–dependent expression of imprinted genes is mostly associated with allele-specific DNA methylation of the CpG islands (CGIs) called germ line differentially methylated regions (gDMRs). Although the essential role of gDMRs for genomic imprinting has been well established, little is kn...

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Autores principales: Suzuki, Shunsuke, Shaw, Geoffrey, Kaneko-Ishino, Tomoko, Ishino, Fumitoshi, Renfree, Marilyn B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3217256/
https://www.ncbi.nlm.nih.gov/pubmed/22016334
http://dx.doi.org/10.1093/gbe/evr104
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author Suzuki, Shunsuke
Shaw, Geoffrey
Kaneko-Ishino, Tomoko
Ishino, Fumitoshi
Renfree, Marilyn B.
author_facet Suzuki, Shunsuke
Shaw, Geoffrey
Kaneko-Ishino, Tomoko
Ishino, Fumitoshi
Renfree, Marilyn B.
author_sort Suzuki, Shunsuke
collection PubMed
description Parent-of-origin–dependent expression of imprinted genes is mostly associated with allele-specific DNA methylation of the CpG islands (CGIs) called germ line differentially methylated regions (gDMRs). Although the essential role of gDMRs for genomic imprinting has been well established, little is known about how they evolved. In several imprinted loci, the CGIs forming gDMRs may have emerged with the insertion of a retrotransposon or retrogene. To examine the generality of the hypothesis that the CGIs forming gDMRs were novel CGIs recently acquired during mammalian evolution, we reviewed the time of novel CGI emergence for all the maternal gDMR loci using the novel data analyzed in this study combined with the data from previous reports. The comparative sequence analyses using mouse, human, dog, cow, elephant, tammar, opossum, platypus, and chicken genomic sequences were carried out for Peg13, Meg1/Grb10, Plagl1/Zac1, Gnas, and Slc38a4 imprinted loci to obtain comprehensive results. The combined data showed that emergence of novel CGIs occurred universally in the maternal gDMR loci at various time points during mammalian evolution. Furthermore, the analysis of Meg1/Grb10 locus provided evidence that gradual base pair–wise sequence change was involved in the accumulation of CpG sequence, suggesting the mechanism of novel CGI emergence is more complex than the suggestion that CpG sequences originated solely by insertion of CpG-rich transposable elements. We propose that acquisition of novel CGIs was a key genomic change for the evolution of imprinting and that it usually occurred in the maternal gDMR loci.
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spelling pubmed-32172562011-11-16 The Evolution of Mammalian Genomic Imprinting Was Accompanied by the Acquisition of Novel CpG Islands Suzuki, Shunsuke Shaw, Geoffrey Kaneko-Ishino, Tomoko Ishino, Fumitoshi Renfree, Marilyn B. Genome Biol Evol Research Articles Parent-of-origin–dependent expression of imprinted genes is mostly associated with allele-specific DNA methylation of the CpG islands (CGIs) called germ line differentially methylated regions (gDMRs). Although the essential role of gDMRs for genomic imprinting has been well established, little is known about how they evolved. In several imprinted loci, the CGIs forming gDMRs may have emerged with the insertion of a retrotransposon or retrogene. To examine the generality of the hypothesis that the CGIs forming gDMRs were novel CGIs recently acquired during mammalian evolution, we reviewed the time of novel CGI emergence for all the maternal gDMR loci using the novel data analyzed in this study combined with the data from previous reports. The comparative sequence analyses using mouse, human, dog, cow, elephant, tammar, opossum, platypus, and chicken genomic sequences were carried out for Peg13, Meg1/Grb10, Plagl1/Zac1, Gnas, and Slc38a4 imprinted loci to obtain comprehensive results. The combined data showed that emergence of novel CGIs occurred universally in the maternal gDMR loci at various time points during mammalian evolution. Furthermore, the analysis of Meg1/Grb10 locus provided evidence that gradual base pair–wise sequence change was involved in the accumulation of CpG sequence, suggesting the mechanism of novel CGI emergence is more complex than the suggestion that CpG sequences originated solely by insertion of CpG-rich transposable elements. We propose that acquisition of novel CGIs was a key genomic change for the evolution of imprinting and that it usually occurred in the maternal gDMR loci. Oxford University Press 2011-10-19 /pmc/articles/PMC3217256/ /pubmed/22016334 http://dx.doi.org/10.1093/gbe/evr104 Text en The Author(s) 2011. Published by Oxford University Press on behalf of the Society for Molecular Biology and Evolution. http://creativecommons.org/licenses/by-nc/3.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0), which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
Suzuki, Shunsuke
Shaw, Geoffrey
Kaneko-Ishino, Tomoko
Ishino, Fumitoshi
Renfree, Marilyn B.
The Evolution of Mammalian Genomic Imprinting Was Accompanied by the Acquisition of Novel CpG Islands
title The Evolution of Mammalian Genomic Imprinting Was Accompanied by the Acquisition of Novel CpG Islands
title_full The Evolution of Mammalian Genomic Imprinting Was Accompanied by the Acquisition of Novel CpG Islands
title_fullStr The Evolution of Mammalian Genomic Imprinting Was Accompanied by the Acquisition of Novel CpG Islands
title_full_unstemmed The Evolution of Mammalian Genomic Imprinting Was Accompanied by the Acquisition of Novel CpG Islands
title_short The Evolution of Mammalian Genomic Imprinting Was Accompanied by the Acquisition of Novel CpG Islands
title_sort evolution of mammalian genomic imprinting was accompanied by the acquisition of novel cpg islands
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3217256/
https://www.ncbi.nlm.nih.gov/pubmed/22016334
http://dx.doi.org/10.1093/gbe/evr104
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