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A Role for ATF2 in Regulating MITF and Melanoma Development

The transcription factor ATF2 has been shown to attenuate melanoma susceptibility to apoptosis and to promote its ability to form tumors in xenograft models. To directly assess ATF2's role in melanoma development, we crossed a mouse melanoma model (Nras(Q61K)::Ink4a(−/−)) with mice expressing a...

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Autores principales: Shah, Meera, Bhoumik, Anindita, Goel, Vikas, Dewing, Antimone, Breitwieser, Wolfgang, Kluger, Harriet, Krajewski, Stan, Krajewska, Maryla, DeHart, Jason, Lau, Eric, Kallenberg, David M., Jeong, Hyeongnam, Eroshkin, Alexey, Bennett, Dorothy C., Chin, Lynda, Bosenberg, Marcus, Jones, Nic, Ronai, Ze'ev A.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3009656/
https://www.ncbi.nlm.nih.gov/pubmed/21203491
http://dx.doi.org/10.1371/journal.pgen.1001258
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author Shah, Meera
Bhoumik, Anindita
Goel, Vikas
Dewing, Antimone
Breitwieser, Wolfgang
Kluger, Harriet
Krajewski, Stan
Krajewska, Maryla
DeHart, Jason
Lau, Eric
Kallenberg, David M.
Jeong, Hyeongnam
Eroshkin, Alexey
Bennett, Dorothy C.
Chin, Lynda
Bosenberg, Marcus
Jones, Nic
Ronai, Ze'ev A.
author_facet Shah, Meera
Bhoumik, Anindita
Goel, Vikas
Dewing, Antimone
Breitwieser, Wolfgang
Kluger, Harriet
Krajewski, Stan
Krajewska, Maryla
DeHart, Jason
Lau, Eric
Kallenberg, David M.
Jeong, Hyeongnam
Eroshkin, Alexey
Bennett, Dorothy C.
Chin, Lynda
Bosenberg, Marcus
Jones, Nic
Ronai, Ze'ev A.
author_sort Shah, Meera
collection PubMed
description The transcription factor ATF2 has been shown to attenuate melanoma susceptibility to apoptosis and to promote its ability to form tumors in xenograft models. To directly assess ATF2's role in melanoma development, we crossed a mouse melanoma model (Nras(Q61K)::Ink4a(−/−)) with mice expressing a transcriptionally inactive form of ATF2 in melanocytes. In contrast to 7/21 of the Nras(Q61K)::Ink4a(−/−) mice, only 1/21 mice expressing mutant ATF2 in melanocytes developed melanoma. Gene expression profiling identified higher MITF expression in primary melanocytes expressing transcriptionally inactive ATF2. MITF downregulation by ATF2 was confirmed in the skin of Atf2(−/−) mice, in primary human melanocytes, and in 50% of human melanoma cell lines. Inhibition of MITF transcription by MITF was shown to be mediated by ATF2-JunB–dependent suppression of SOX10 transcription. Remarkably, oncogenic BRAF (V600E)–dependent focus formation of melanocytes on soft agar was inhibited by ATF2 knockdown and partially rescued upon shMITF co-expression. On melanoma tissue microarrays, a high nuclear ATF2 to MITF ratio in primary specimens was associated with metastatic disease and poor prognosis. Our findings establish the importance of transcriptionally active ATF2 in melanoma development through fine-tuning of MITF expression.
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spelling pubmed-30096562011-01-03 A Role for ATF2 in Regulating MITF and Melanoma Development Shah, Meera Bhoumik, Anindita Goel, Vikas Dewing, Antimone Breitwieser, Wolfgang Kluger, Harriet Krajewski, Stan Krajewska, Maryla DeHart, Jason Lau, Eric Kallenberg, David M. Jeong, Hyeongnam Eroshkin, Alexey Bennett, Dorothy C. Chin, Lynda Bosenberg, Marcus Jones, Nic Ronai, Ze'ev A. PLoS Genet Research Article The transcription factor ATF2 has been shown to attenuate melanoma susceptibility to apoptosis and to promote its ability to form tumors in xenograft models. To directly assess ATF2's role in melanoma development, we crossed a mouse melanoma model (Nras(Q61K)::Ink4a(−/−)) with mice expressing a transcriptionally inactive form of ATF2 in melanocytes. In contrast to 7/21 of the Nras(Q61K)::Ink4a(−/−) mice, only 1/21 mice expressing mutant ATF2 in melanocytes developed melanoma. Gene expression profiling identified higher MITF expression in primary melanocytes expressing transcriptionally inactive ATF2. MITF downregulation by ATF2 was confirmed in the skin of Atf2(−/−) mice, in primary human melanocytes, and in 50% of human melanoma cell lines. Inhibition of MITF transcription by MITF was shown to be mediated by ATF2-JunB–dependent suppression of SOX10 transcription. Remarkably, oncogenic BRAF (V600E)–dependent focus formation of melanocytes on soft agar was inhibited by ATF2 knockdown and partially rescued upon shMITF co-expression. On melanoma tissue microarrays, a high nuclear ATF2 to MITF ratio in primary specimens was associated with metastatic disease and poor prognosis. Our findings establish the importance of transcriptionally active ATF2 in melanoma development through fine-tuning of MITF expression. Public Library of Science 2010-12-23 /pmc/articles/PMC3009656/ /pubmed/21203491 http://dx.doi.org/10.1371/journal.pgen.1001258 Text en Shah 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
Shah, Meera
Bhoumik, Anindita
Goel, Vikas
Dewing, Antimone
Breitwieser, Wolfgang
Kluger, Harriet
Krajewski, Stan
Krajewska, Maryla
DeHart, Jason
Lau, Eric
Kallenberg, David M.
Jeong, Hyeongnam
Eroshkin, Alexey
Bennett, Dorothy C.
Chin, Lynda
Bosenberg, Marcus
Jones, Nic
Ronai, Ze'ev A.
A Role for ATF2 in Regulating MITF and Melanoma Development
title A Role for ATF2 in Regulating MITF and Melanoma Development
title_full A Role for ATF2 in Regulating MITF and Melanoma Development
title_fullStr A Role for ATF2 in Regulating MITF and Melanoma Development
title_full_unstemmed A Role for ATF2 in Regulating MITF and Melanoma Development
title_short A Role for ATF2 in Regulating MITF and Melanoma Development
title_sort role for atf2 in regulating mitf and melanoma development
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3009656/
https://www.ncbi.nlm.nih.gov/pubmed/21203491
http://dx.doi.org/10.1371/journal.pgen.1001258
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