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Identification of a Novel C-Terminal Truncated WT1 Isoform with Antagonistic Effects against Major WT1 Isoforms

The Wilms’ tumor gene WT1 consists of 10 exons and encodes a zinc finger transcription factor. There are four major WT1 isoforms resulting from alternative splicing at two sites, exon 5 (17AA) and exon 9 (KTS). All major WT1 isoforms are overexpressed in leukemia and solid tumors and play oncogenic...

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Autores principales: Tatsumi, Naoya, Hojo, Nozomi, Sakamoto, Hiroyuki, Inaba, Rena, Moriguchi, Nahoko, Matsuno, Keiko, Fukuda, Mari, Matsumura, Akihide, Hayashi, Seiji, Morimoto, Soyoko, Nakata, Jun, Fujiki, Fumihiro, Nishida, Sumiyuki, Nakajima, Hiroko, Tsuboi, Akihiro, Oka, Yoshihiro, Hosen, Naoki, Sugiyama, Haruo, Oji, Yusuke
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4474557/
https://www.ncbi.nlm.nih.gov/pubmed/26090994
http://dx.doi.org/10.1371/journal.pone.0130578
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author Tatsumi, Naoya
Hojo, Nozomi
Sakamoto, Hiroyuki
Inaba, Rena
Moriguchi, Nahoko
Matsuno, Keiko
Fukuda, Mari
Matsumura, Akihide
Hayashi, Seiji
Morimoto, Soyoko
Nakata, Jun
Fujiki, Fumihiro
Nishida, Sumiyuki
Nakajima, Hiroko
Tsuboi, Akihiro
Oka, Yoshihiro
Hosen, Naoki
Sugiyama, Haruo
Oji, Yusuke
author_facet Tatsumi, Naoya
Hojo, Nozomi
Sakamoto, Hiroyuki
Inaba, Rena
Moriguchi, Nahoko
Matsuno, Keiko
Fukuda, Mari
Matsumura, Akihide
Hayashi, Seiji
Morimoto, Soyoko
Nakata, Jun
Fujiki, Fumihiro
Nishida, Sumiyuki
Nakajima, Hiroko
Tsuboi, Akihiro
Oka, Yoshihiro
Hosen, Naoki
Sugiyama, Haruo
Oji, Yusuke
author_sort Tatsumi, Naoya
collection PubMed
description The Wilms’ tumor gene WT1 consists of 10 exons and encodes a zinc finger transcription factor. There are four major WT1 isoforms resulting from alternative splicing at two sites, exon 5 (17AA) and exon 9 (KTS). All major WT1 isoforms are overexpressed in leukemia and solid tumors and play oncogenic roles such as inhibition of apoptosis, and promotion of cell proliferation, migration and invasion. In the present study, a novel alternatively spliced WT1 isoform that had an extended exon 4 (designated as exon 4a) with an additional 153 bp (designated as 4a sequence) at the 3’ end was identified and designated as an Ex4a(+)WT1 isoform. The insertion of exon 4a resulted in the introduction of premature translational stop codons in the reading frame in exon 4a and production of C-terminal truncated WT1 proteins lacking zinc finger DNA-binding domain. Overexpression of the truncated Ex4a(+)WT1 isoform inhibited the major WT1-mediated transcriptional activation of anti-apoptotic Bcl-xL gene promoter and induced mitochondrial damage and apoptosis. Conversely, suppression of the Ex4a(+)WT1 isoform by Ex4a-specific siRNA attenuated apoptosis. These results indicated that the Ex4a(+)WT1 isoform exerted dominant negative effects on anti-apoptotic function of major WT1 isoforms. Ex4a(+)WT1 isoform was endogenously expressed as a minor isoform in myeloid leukemia and solid tumor cells and increased regardless of decrease in major WT1 isoforms during apoptosis, suggesting the dominant negative effects on anti-apoptotic function of major WT1 isoforms. These results indicated that Ex4a(+)WT1 isoform had an important physiological function that regulated oncogenic function of major WT1 isoforms.
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spelling pubmed-44745572015-06-30 Identification of a Novel C-Terminal Truncated WT1 Isoform with Antagonistic Effects against Major WT1 Isoforms Tatsumi, Naoya Hojo, Nozomi Sakamoto, Hiroyuki Inaba, Rena Moriguchi, Nahoko Matsuno, Keiko Fukuda, Mari Matsumura, Akihide Hayashi, Seiji Morimoto, Soyoko Nakata, Jun Fujiki, Fumihiro Nishida, Sumiyuki Nakajima, Hiroko Tsuboi, Akihiro Oka, Yoshihiro Hosen, Naoki Sugiyama, Haruo Oji, Yusuke PLoS One Research Article The Wilms’ tumor gene WT1 consists of 10 exons and encodes a zinc finger transcription factor. There are four major WT1 isoforms resulting from alternative splicing at two sites, exon 5 (17AA) and exon 9 (KTS). All major WT1 isoforms are overexpressed in leukemia and solid tumors and play oncogenic roles such as inhibition of apoptosis, and promotion of cell proliferation, migration and invasion. In the present study, a novel alternatively spliced WT1 isoform that had an extended exon 4 (designated as exon 4a) with an additional 153 bp (designated as 4a sequence) at the 3’ end was identified and designated as an Ex4a(+)WT1 isoform. The insertion of exon 4a resulted in the introduction of premature translational stop codons in the reading frame in exon 4a and production of C-terminal truncated WT1 proteins lacking zinc finger DNA-binding domain. Overexpression of the truncated Ex4a(+)WT1 isoform inhibited the major WT1-mediated transcriptional activation of anti-apoptotic Bcl-xL gene promoter and induced mitochondrial damage and apoptosis. Conversely, suppression of the Ex4a(+)WT1 isoform by Ex4a-specific siRNA attenuated apoptosis. These results indicated that the Ex4a(+)WT1 isoform exerted dominant negative effects on anti-apoptotic function of major WT1 isoforms. Ex4a(+)WT1 isoform was endogenously expressed as a minor isoform in myeloid leukemia and solid tumor cells and increased regardless of decrease in major WT1 isoforms during apoptosis, suggesting the dominant negative effects on anti-apoptotic function of major WT1 isoforms. These results indicated that Ex4a(+)WT1 isoform had an important physiological function that regulated oncogenic function of major WT1 isoforms. Public Library of Science 2015-06-19 /pmc/articles/PMC4474557/ /pubmed/26090994 http://dx.doi.org/10.1371/journal.pone.0130578 Text en © 2015 Tatsumi 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
Tatsumi, Naoya
Hojo, Nozomi
Sakamoto, Hiroyuki
Inaba, Rena
Moriguchi, Nahoko
Matsuno, Keiko
Fukuda, Mari
Matsumura, Akihide
Hayashi, Seiji
Morimoto, Soyoko
Nakata, Jun
Fujiki, Fumihiro
Nishida, Sumiyuki
Nakajima, Hiroko
Tsuboi, Akihiro
Oka, Yoshihiro
Hosen, Naoki
Sugiyama, Haruo
Oji, Yusuke
Identification of a Novel C-Terminal Truncated WT1 Isoform with Antagonistic Effects against Major WT1 Isoforms
title Identification of a Novel C-Terminal Truncated WT1 Isoform with Antagonistic Effects against Major WT1 Isoforms
title_full Identification of a Novel C-Terminal Truncated WT1 Isoform with Antagonistic Effects against Major WT1 Isoforms
title_fullStr Identification of a Novel C-Terminal Truncated WT1 Isoform with Antagonistic Effects against Major WT1 Isoforms
title_full_unstemmed Identification of a Novel C-Terminal Truncated WT1 Isoform with Antagonistic Effects against Major WT1 Isoforms
title_short Identification of a Novel C-Terminal Truncated WT1 Isoform with Antagonistic Effects against Major WT1 Isoforms
title_sort identification of a novel c-terminal truncated wt1 isoform with antagonistic effects against major wt1 isoforms
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4474557/
https://www.ncbi.nlm.nih.gov/pubmed/26090994
http://dx.doi.org/10.1371/journal.pone.0130578
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