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Gene Mutations and Genomic Rearrangements in the Mouse as a Result of Transposon Mobilization from Chromosomal Concatemers

Previous studies of the Sleeping Beauty (SB) transposon system, as an insertional mutagen in the germline of mice, have used reverse genetic approaches. These studies have led to its proposed use for regional saturation mutagenesis by taking a forward-genetic approach. Thus, we used the SB system to...

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Autores principales: Geurts, Aron M, Collier, Lara S, Geurts, Jennifer L, Oseth, Leann L, Bell, Matthew L, Mu, David, Lucito, Robert, Godbout, Susan A, Green, Laura E, Lowe, Scott W, Hirsch, Betsy A, Leinwand, Leslie A, Largaespada, David A
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2006
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1584263/
https://www.ncbi.nlm.nih.gov/pubmed/17009875
http://dx.doi.org/10.1371/journal.pgen.0020156
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author Geurts, Aron M
Collier, Lara S
Geurts, Jennifer L
Oseth, Leann L
Bell, Matthew L
Mu, David
Lucito, Robert
Godbout, Susan A
Green, Laura E
Lowe, Scott W
Hirsch, Betsy A
Leinwand, Leslie A
Largaespada, David A
author_facet Geurts, Aron M
Collier, Lara S
Geurts, Jennifer L
Oseth, Leann L
Bell, Matthew L
Mu, David
Lucito, Robert
Godbout, Susan A
Green, Laura E
Lowe, Scott W
Hirsch, Betsy A
Leinwand, Leslie A
Largaespada, David A
author_sort Geurts, Aron M
collection PubMed
description Previous studies of the Sleeping Beauty (SB) transposon system, as an insertional mutagen in the germline of mice, have used reverse genetic approaches. These studies have led to its proposed use for regional saturation mutagenesis by taking a forward-genetic approach. Thus, we used the SB system to mutate a region of mouse Chromosome 11 in a forward-genetic screen for recessive lethal and viable phenotypes. This work represents the first reported use of an insertional mutagen in a phenotype-driven approach. The phenotype-driven approach was successful in both recovering visible and behavioral mutants, including dominant limb and recessive behavioral phenotypes, and allowing for the rapid identification of candidate gene disruptions. In addition, a high frequency of recessive lethal mutations arose as a result of genomic rearrangements near the site of transposition, resulting from transposon mobilization. The results suggest that the SB system could be used in a forward-genetic approach to recover interesting phenotypes, but that local chromosomal rearrangements should be anticipated in conjunction with single-copy, local transposon insertions in chromosomes. Additionally, these mice may serve as a model for chromosome rearrangements caused by transposable elements during the evolution of vertebrate genomes.
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spelling pubmed-15842632006-10-05 Gene Mutations and Genomic Rearrangements in the Mouse as a Result of Transposon Mobilization from Chromosomal Concatemers Geurts, Aron M Collier, Lara S Geurts, Jennifer L Oseth, Leann L Bell, Matthew L Mu, David Lucito, Robert Godbout, Susan A Green, Laura E Lowe, Scott W Hirsch, Betsy A Leinwand, Leslie A Largaespada, David A PLoS Genet Research Article Previous studies of the Sleeping Beauty (SB) transposon system, as an insertional mutagen in the germline of mice, have used reverse genetic approaches. These studies have led to its proposed use for regional saturation mutagenesis by taking a forward-genetic approach. Thus, we used the SB system to mutate a region of mouse Chromosome 11 in a forward-genetic screen for recessive lethal and viable phenotypes. This work represents the first reported use of an insertional mutagen in a phenotype-driven approach. The phenotype-driven approach was successful in both recovering visible and behavioral mutants, including dominant limb and recessive behavioral phenotypes, and allowing for the rapid identification of candidate gene disruptions. In addition, a high frequency of recessive lethal mutations arose as a result of genomic rearrangements near the site of transposition, resulting from transposon mobilization. The results suggest that the SB system could be used in a forward-genetic approach to recover interesting phenotypes, but that local chromosomal rearrangements should be anticipated in conjunction with single-copy, local transposon insertions in chromosomes. Additionally, these mice may serve as a model for chromosome rearrangements caused by transposable elements during the evolution of vertebrate genomes. Public Library of Science 2006-09 2006-09-29 /pmc/articles/PMC1584263/ /pubmed/17009875 http://dx.doi.org/10.1371/journal.pgen.0020156 Text en © 2006 Geurts 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
Geurts, Aron M
Collier, Lara S
Geurts, Jennifer L
Oseth, Leann L
Bell, Matthew L
Mu, David
Lucito, Robert
Godbout, Susan A
Green, Laura E
Lowe, Scott W
Hirsch, Betsy A
Leinwand, Leslie A
Largaespada, David A
Gene Mutations and Genomic Rearrangements in the Mouse as a Result of Transposon Mobilization from Chromosomal Concatemers
title Gene Mutations and Genomic Rearrangements in the Mouse as a Result of Transposon Mobilization from Chromosomal Concatemers
title_full Gene Mutations and Genomic Rearrangements in the Mouse as a Result of Transposon Mobilization from Chromosomal Concatemers
title_fullStr Gene Mutations and Genomic Rearrangements in the Mouse as a Result of Transposon Mobilization from Chromosomal Concatemers
title_full_unstemmed Gene Mutations and Genomic Rearrangements in the Mouse as a Result of Transposon Mobilization from Chromosomal Concatemers
title_short Gene Mutations and Genomic Rearrangements in the Mouse as a Result of Transposon Mobilization from Chromosomal Concatemers
title_sort gene mutations and genomic rearrangements in the mouse as a result of transposon mobilization from chromosomal concatemers
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1584263/
https://www.ncbi.nlm.nih.gov/pubmed/17009875
http://dx.doi.org/10.1371/journal.pgen.0020156
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