BRN2 suppresses apoptosis, reprograms DNA damage repair, and is associated with a high somatic mutation burden in melanoma

Whether cell types exposed to a high level of environmental insults possess cell type-specific prosurvival mechanisms or enhanced DNA damage repair capacity is not well understood. BRN2 is a tissue-restricted POU domain transcription factor implicated in neural development and several cancers. In me...

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Autores principales: Herbert, Katharine, Binet, Romuald, Lambert, Jean-Philippe, Louphrasitthiphol, Pakavarin, Kalkavan, Halime, Sesma-Sanz, Laura, Robles-Espinoza, Carla Daniela, Sarkar, Sovan, Suer, Eda, Andrews, Sarah, Chauhan, Jagat, Roberts, Nicola D., Middleton, Mark R., Gingras, Anne-Claude, Masson, Jean-Yves, Larue, Lionel, Falletta, Paola, Goding, Colin R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory Press 2019
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6411009/
https://www.ncbi.nlm.nih.gov/pubmed/30804224
http://dx.doi.org/10.1101/gad.314633.118
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author Herbert, Katharine
Binet, Romuald
Lambert, Jean-Philippe
Louphrasitthiphol, Pakavarin
Kalkavan, Halime
Sesma-Sanz, Laura
Robles-Espinoza, Carla Daniela
Sarkar, Sovan
Suer, Eda
Andrews, Sarah
Chauhan, Jagat
Roberts, Nicola D.
Middleton, Mark R.
Gingras, Anne-Claude
Masson, Jean-Yves
Larue, Lionel
Falletta, Paola
Goding, Colin R.
author_facet Herbert, Katharine
Binet, Romuald
Lambert, Jean-Philippe
Louphrasitthiphol, Pakavarin
Kalkavan, Halime
Sesma-Sanz, Laura
Robles-Espinoza, Carla Daniela
Sarkar, Sovan
Suer, Eda
Andrews, Sarah
Chauhan, Jagat
Roberts, Nicola D.
Middleton, Mark R.
Gingras, Anne-Claude
Masson, Jean-Yves
Larue, Lionel
Falletta, Paola
Goding, Colin R.
author_sort Herbert, Katharine
collection PubMed
description Whether cell types exposed to a high level of environmental insults possess cell type-specific prosurvival mechanisms or enhanced DNA damage repair capacity is not well understood. BRN2 is a tissue-restricted POU domain transcription factor implicated in neural development and several cancers. In melanoma, BRN2 plays a key role in promoting invasion and regulating proliferation. Here we found, surprisingly, that rather than interacting with transcription cofactors, BRN2 is instead associated with DNA damage response proteins and directly binds PARP1 and Ku70/Ku80. Rapid PARP1-dependent BRN2 association with sites of DNA damage facilitates recruitment of Ku80 and reprograms DNA damage repair by promoting Ku-dependent nonhomologous end-joining (NHEJ) at the expense of homologous recombination. BRN2 also suppresses an apoptosis-associated gene expression program to protect against UVB-, chemotherapy- and vemurafenib-induced apoptosis. Remarkably, BRN2 expression also correlates with a high single-nucleotide variation prevalence in human melanomas. By promoting error-prone DNA damage repair via NHEJ and suppressing apoptosis of damaged cells, our results suggest that BRN2 contributes to the generation of melanomas with a high mutation burden. Our findings highlight a novel role for a key transcription factor in reprogramming DNA damage repair and suggest that BRN2 may impact the response to DNA-damaging agents in BRN2-expressing cancers.
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spelling pubmed-64110092019-03-27 BRN2 suppresses apoptosis, reprograms DNA damage repair, and is associated with a high somatic mutation burden in melanoma Herbert, Katharine Binet, Romuald Lambert, Jean-Philippe Louphrasitthiphol, Pakavarin Kalkavan, Halime Sesma-Sanz, Laura Robles-Espinoza, Carla Daniela Sarkar, Sovan Suer, Eda Andrews, Sarah Chauhan, Jagat Roberts, Nicola D. Middleton, Mark R. Gingras, Anne-Claude Masson, Jean-Yves Larue, Lionel Falletta, Paola Goding, Colin R. Genes Dev Research Paper Whether cell types exposed to a high level of environmental insults possess cell type-specific prosurvival mechanisms or enhanced DNA damage repair capacity is not well understood. BRN2 is a tissue-restricted POU domain transcription factor implicated in neural development and several cancers. In melanoma, BRN2 plays a key role in promoting invasion and regulating proliferation. Here we found, surprisingly, that rather than interacting with transcription cofactors, BRN2 is instead associated with DNA damage response proteins and directly binds PARP1 and Ku70/Ku80. Rapid PARP1-dependent BRN2 association with sites of DNA damage facilitates recruitment of Ku80 and reprograms DNA damage repair by promoting Ku-dependent nonhomologous end-joining (NHEJ) at the expense of homologous recombination. BRN2 also suppresses an apoptosis-associated gene expression program to protect against UVB-, chemotherapy- and vemurafenib-induced apoptosis. Remarkably, BRN2 expression also correlates with a high single-nucleotide variation prevalence in human melanomas. By promoting error-prone DNA damage repair via NHEJ and suppressing apoptosis of damaged cells, our results suggest that BRN2 contributes to the generation of melanomas with a high mutation burden. Our findings highlight a novel role for a key transcription factor in reprogramming DNA damage repair and suggest that BRN2 may impact the response to DNA-damaging agents in BRN2-expressing cancers. Cold Spring Harbor Laboratory Press 2019-03-01 /pmc/articles/PMC6411009/ /pubmed/30804224 http://dx.doi.org/10.1101/gad.314633.118 Text en © 2019 Herbert et al.; Published by Cold Spring Harbor Laboratory Press http://creativecommons.org/licenses/by/4.0/ This article, published in Genes & Development, is available under a Creative Commons License (Attribution 4.0 International), as described at http://creativecommons.org/licenses/by/4.0/.
spellingShingle Research Paper
Herbert, Katharine
Binet, Romuald
Lambert, Jean-Philippe
Louphrasitthiphol, Pakavarin
Kalkavan, Halime
Sesma-Sanz, Laura
Robles-Espinoza, Carla Daniela
Sarkar, Sovan
Suer, Eda
Andrews, Sarah
Chauhan, Jagat
Roberts, Nicola D.
Middleton, Mark R.
Gingras, Anne-Claude
Masson, Jean-Yves
Larue, Lionel
Falletta, Paola
Goding, Colin R.
BRN2 suppresses apoptosis, reprograms DNA damage repair, and is associated with a high somatic mutation burden in melanoma
title BRN2 suppresses apoptosis, reprograms DNA damage repair, and is associated with a high somatic mutation burden in melanoma
title_full BRN2 suppresses apoptosis, reprograms DNA damage repair, and is associated with a high somatic mutation burden in melanoma
title_fullStr BRN2 suppresses apoptosis, reprograms DNA damage repair, and is associated with a high somatic mutation burden in melanoma
title_full_unstemmed BRN2 suppresses apoptosis, reprograms DNA damage repair, and is associated with a high somatic mutation burden in melanoma
title_short BRN2 suppresses apoptosis, reprograms DNA damage repair, and is associated with a high somatic mutation burden in melanoma
title_sort brn2 suppresses apoptosis, reprograms dna damage repair, and is associated with a high somatic mutation burden in melanoma
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6411009/
https://www.ncbi.nlm.nih.gov/pubmed/30804224
http://dx.doi.org/10.1101/gad.314633.118
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