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A Comprehensive Map of Mobile Element Insertion Polymorphisms in Humans

As a consequence of the accumulation of insertion events over evolutionary time, mobile elements now comprise nearly half of the human genome. The Alu, L1, and SVA mobile element families are still duplicating, generating variation between individual genomes. Mobile element insertions (MEI) have bee...

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Autores principales: Stewart, Chip, Kural, Deniz, Strömberg, Michael P., Walker, Jerilyn A., Konkel, Miriam K., Stütz, Adrian M., Urban, Alexander E., Grubert, Fabian, Lam, Hugo Y. K., Lee, Wan-Ping, Busby, Michele, Indap, Amit R., Garrison, Erik, Huff, Chad, Xing, Jinchuan, Snyder, Michael P., Jorde, Lynn B., Batzer, Mark A., Korbel, Jan O., Marth, Gabor T.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3158055/
https://www.ncbi.nlm.nih.gov/pubmed/21876680
http://dx.doi.org/10.1371/journal.pgen.1002236
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author Stewart, Chip
Kural, Deniz
Strömberg, Michael P.
Walker, Jerilyn A.
Konkel, Miriam K.
Stütz, Adrian M.
Urban, Alexander E.
Grubert, Fabian
Lam, Hugo Y. K.
Lee, Wan-Ping
Busby, Michele
Indap, Amit R.
Garrison, Erik
Huff, Chad
Xing, Jinchuan
Snyder, Michael P.
Jorde, Lynn B.
Batzer, Mark A.
Korbel, Jan O.
Marth, Gabor T.
author_facet Stewart, Chip
Kural, Deniz
Strömberg, Michael P.
Walker, Jerilyn A.
Konkel, Miriam K.
Stütz, Adrian M.
Urban, Alexander E.
Grubert, Fabian
Lam, Hugo Y. K.
Lee, Wan-Ping
Busby, Michele
Indap, Amit R.
Garrison, Erik
Huff, Chad
Xing, Jinchuan
Snyder, Michael P.
Jorde, Lynn B.
Batzer, Mark A.
Korbel, Jan O.
Marth, Gabor T.
author_sort Stewart, Chip
collection PubMed
description As a consequence of the accumulation of insertion events over evolutionary time, mobile elements now comprise nearly half of the human genome. The Alu, L1, and SVA mobile element families are still duplicating, generating variation between individual genomes. Mobile element insertions (MEI) have been identified as causes for genetic diseases, including hemophilia, neurofibromatosis, and various cancers. Here we present a comprehensive map of 7,380 MEI polymorphisms from the 1000 Genomes Project whole-genome sequencing data of 185 samples in three major populations detected with two detection methods. This catalog enables us to systematically study mutation rates, population segregation, genomic distribution, and functional properties of MEI polymorphisms and to compare MEI to SNP variation from the same individuals. Population allele frequencies of MEI and SNPs are described, broadly, by the same neutral ancestral processes despite vastly different mutation mechanisms and rates, except in coding regions where MEI are virtually absent, presumably due to strong negative selection. A direct comparison of MEI and SNP diversity levels suggests a differential mobile element insertion rate among populations.
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spelling pubmed-31580552011-08-29 A Comprehensive Map of Mobile Element Insertion Polymorphisms in Humans Stewart, Chip Kural, Deniz Strömberg, Michael P. Walker, Jerilyn A. Konkel, Miriam K. Stütz, Adrian M. Urban, Alexander E. Grubert, Fabian Lam, Hugo Y. K. Lee, Wan-Ping Busby, Michele Indap, Amit R. Garrison, Erik Huff, Chad Xing, Jinchuan Snyder, Michael P. Jorde, Lynn B. Batzer, Mark A. Korbel, Jan O. Marth, Gabor T. PLoS Genet Research Article As a consequence of the accumulation of insertion events over evolutionary time, mobile elements now comprise nearly half of the human genome. The Alu, L1, and SVA mobile element families are still duplicating, generating variation between individual genomes. Mobile element insertions (MEI) have been identified as causes for genetic diseases, including hemophilia, neurofibromatosis, and various cancers. Here we present a comprehensive map of 7,380 MEI polymorphisms from the 1000 Genomes Project whole-genome sequencing data of 185 samples in three major populations detected with two detection methods. This catalog enables us to systematically study mutation rates, population segregation, genomic distribution, and functional properties of MEI polymorphisms and to compare MEI to SNP variation from the same individuals. Population allele frequencies of MEI and SNPs are described, broadly, by the same neutral ancestral processes despite vastly different mutation mechanisms and rates, except in coding regions where MEI are virtually absent, presumably due to strong negative selection. A direct comparison of MEI and SNP diversity levels suggests a differential mobile element insertion rate among populations. Public Library of Science 2011-08-18 /pmc/articles/PMC3158055/ /pubmed/21876680 http://dx.doi.org/10.1371/journal.pgen.1002236 Text en Stewart 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
Stewart, Chip
Kural, Deniz
Strömberg, Michael P.
Walker, Jerilyn A.
Konkel, Miriam K.
Stütz, Adrian M.
Urban, Alexander E.
Grubert, Fabian
Lam, Hugo Y. K.
Lee, Wan-Ping
Busby, Michele
Indap, Amit R.
Garrison, Erik
Huff, Chad
Xing, Jinchuan
Snyder, Michael P.
Jorde, Lynn B.
Batzer, Mark A.
Korbel, Jan O.
Marth, Gabor T.
A Comprehensive Map of Mobile Element Insertion Polymorphisms in Humans
title A Comprehensive Map of Mobile Element Insertion Polymorphisms in Humans
title_full A Comprehensive Map of Mobile Element Insertion Polymorphisms in Humans
title_fullStr A Comprehensive Map of Mobile Element Insertion Polymorphisms in Humans
title_full_unstemmed A Comprehensive Map of Mobile Element Insertion Polymorphisms in Humans
title_short A Comprehensive Map of Mobile Element Insertion Polymorphisms in Humans
title_sort comprehensive map of mobile element insertion polymorphisms in humans
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3158055/
https://www.ncbi.nlm.nih.gov/pubmed/21876680
http://dx.doi.org/10.1371/journal.pgen.1002236
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