A novel intergenic ETnII-β insertion mutation causes multiple malformations in polypodia mice.
Mouse early transposon insertions are responsible for ~10% of spontaneous mutant phenotypes. We previously reported the phenotypes and genetic mapping of Polypodia, (Ppd), a spontaneous, X-linked dominant mutation with profound effects on body plan morphogenesis. Our new data shows that mutant mice...
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Public Library of Science (PLoS)
2013-01-01
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| Series: | PLoS Genetics |
| Online Access: | http://europepmc.org/articles/PMC3854779?pdf=render |
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doaj-7e2168f239154d7b8e912471175439002020-11-25T01:32:48ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042013-01-01912e100396710.1371/journal.pgen.1003967A novel intergenic ETnII-β insertion mutation causes multiple malformations in polypodia mice.Jessica A LehoczkyPeedikayil E ThomasKevin M PatrieKailey M OwensLisa M VillarrealKenneth GalbraithJoe WashburnCraig N JohnsonBryant GavinoAlexander D BorowskyKathleen J MillenPaul WakenightWilliam LawMargaret L Van KeurenGalina GavrilinaElizabeth D HughesThomas L SaundersLesil BrihnJoseph H NadeauJeffrey W InnisMouse early transposon insertions are responsible for ~10% of spontaneous mutant phenotypes. We previously reported the phenotypes and genetic mapping of Polypodia, (Ppd), a spontaneous, X-linked dominant mutation with profound effects on body plan morphogenesis. Our new data shows that mutant mice are not born in expected Mendelian ratios secondary to loss after E9.5. In addition, we refined the Ppd genetic interval and discovered a novel ETnII-β early transposon insertion between the genes for Dusp9 and Pnck. The ETn inserted 1.6 kb downstream and antisense to Dusp9 and does not disrupt polyadenylation or splicing of either gene. Knock-in mice engineered to carry the ETn display Ppd characteristic ectopic caudal limb phenotypes, showing that the ETn insertion is the Ppd molecular lesion. Early transposons are actively expressed in the early blastocyst. To explore the consequences of the ETn on the genomic landscape at an early stage of development, we compared interval gene expression between wild-type and mutant ES cells. Mutant ES cell expression analysis revealed marked upregulation of Dusp9 mRNA and protein expression. Evaluation of the 5' LTR CpG methylation state in adult mice revealed no correlation with the occurrence or severity of Ppd phenotypes at birth. Thus, the broad range of phenotypes observed in this mutant is secondary to a novel intergenic ETn insertion whose effects include dysregulation of nearby interval gene expression at early stages of development.http://europepmc.org/articles/PMC3854779?pdf=render |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Jessica A Lehoczky Peedikayil E Thomas Kevin M Patrie Kailey M Owens Lisa M Villarreal Kenneth Galbraith Joe Washburn Craig N Johnson Bryant Gavino Alexander D Borowsky Kathleen J Millen Paul Wakenight William Law Margaret L Van Keuren Galina Gavrilina Elizabeth D Hughes Thomas L Saunders Lesil Brihn Joseph H Nadeau Jeffrey W Innis |
| spellingShingle |
Jessica A Lehoczky Peedikayil E Thomas Kevin M Patrie Kailey M Owens Lisa M Villarreal Kenneth Galbraith Joe Washburn Craig N Johnson Bryant Gavino Alexander D Borowsky Kathleen J Millen Paul Wakenight William Law Margaret L Van Keuren Galina Gavrilina Elizabeth D Hughes Thomas L Saunders Lesil Brihn Joseph H Nadeau Jeffrey W Innis A novel intergenic ETnII-β insertion mutation causes multiple malformations in polypodia mice. PLoS Genetics |
| author_facet |
Jessica A Lehoczky Peedikayil E Thomas Kevin M Patrie Kailey M Owens Lisa M Villarreal Kenneth Galbraith Joe Washburn Craig N Johnson Bryant Gavino Alexander D Borowsky Kathleen J Millen Paul Wakenight William Law Margaret L Van Keuren Galina Gavrilina Elizabeth D Hughes Thomas L Saunders Lesil Brihn Joseph H Nadeau Jeffrey W Innis |
| author_sort |
Jessica A Lehoczky |
| title |
A novel intergenic ETnII-β insertion mutation causes multiple malformations in polypodia mice. |
| title_short |
A novel intergenic ETnII-β insertion mutation causes multiple malformations in polypodia mice. |
| title_full |
A novel intergenic ETnII-β insertion mutation causes multiple malformations in polypodia mice. |
| title_fullStr |
A novel intergenic ETnII-β insertion mutation causes multiple malformations in polypodia mice. |
| title_full_unstemmed |
A novel intergenic ETnII-β insertion mutation causes multiple malformations in polypodia mice. |
| title_sort |
novel intergenic etnii-β insertion mutation causes multiple malformations in polypodia mice. |
| publisher |
Public Library of Science (PLoS) |
| series |
PLoS Genetics |
| issn |
1553-7390 1553-7404 |
| publishDate |
2013-01-01 |
| description |
Mouse early transposon insertions are responsible for ~10% of spontaneous mutant phenotypes. We previously reported the phenotypes and genetic mapping of Polypodia, (Ppd), a spontaneous, X-linked dominant mutation with profound effects on body plan morphogenesis. Our new data shows that mutant mice are not born in expected Mendelian ratios secondary to loss after E9.5. In addition, we refined the Ppd genetic interval and discovered a novel ETnII-β early transposon insertion between the genes for Dusp9 and Pnck. The ETn inserted 1.6 kb downstream and antisense to Dusp9 and does not disrupt polyadenylation or splicing of either gene. Knock-in mice engineered to carry the ETn display Ppd characteristic ectopic caudal limb phenotypes, showing that the ETn insertion is the Ppd molecular lesion. Early transposons are actively expressed in the early blastocyst. To explore the consequences of the ETn on the genomic landscape at an early stage of development, we compared interval gene expression between wild-type and mutant ES cells. Mutant ES cell expression analysis revealed marked upregulation of Dusp9 mRNA and protein expression. Evaluation of the 5' LTR CpG methylation state in adult mice revealed no correlation with the occurrence or severity of Ppd phenotypes at birth. Thus, the broad range of phenotypes observed in this mutant is secondary to a novel intergenic ETn insertion whose effects include dysregulation of nearby interval gene expression at early stages of development. |
| url |
http://europepmc.org/articles/PMC3854779?pdf=render |
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