IRAK1 is a novel DEK transcriptional target and is essential for head and neck cancer cell survival

The chromatin-binding DEK protein was recently reported to promote the growth of HPV(+) and HPV(−) head and neck squamous cell carcinomas (HNSCCs). Relevant cellular and molecular mechanism(s) controlled by DEK in HNSCC remain poorly understood. While DEK is known to regulate specific transcriptiona...

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Autores principales: Adams, Allie K., Bolanos, Lyndsey C., Dexheimer, Phillip J., Karns, Rebekah A., Aronow, Bruce J., Komurov, Kakajan, Jegga, Anil G., Casper, Keith A., Patil, Yash J., Wilson, Keith M., Starczynowski, Daniel T., Wells, Susanne I.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4791239/
https://www.ncbi.nlm.nih.gov/pubmed/26527316
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author Adams, Allie K.
Bolanos, Lyndsey C.
Dexheimer, Phillip J.
Karns, Rebekah A.
Aronow, Bruce J.
Komurov, Kakajan
Jegga, Anil G.
Casper, Keith A.
Patil, Yash J.
Wilson, Keith M.
Starczynowski, Daniel T.
Wells, Susanne I.
author_facet Adams, Allie K.
Bolanos, Lyndsey C.
Dexheimer, Phillip J.
Karns, Rebekah A.
Aronow, Bruce J.
Komurov, Kakajan
Jegga, Anil G.
Casper, Keith A.
Patil, Yash J.
Wilson, Keith M.
Starczynowski, Daniel T.
Wells, Susanne I.
author_sort Adams, Allie K.
collection PubMed
description The chromatin-binding DEK protein was recently reported to promote the growth of HPV(+) and HPV(−) head and neck squamous cell carcinomas (HNSCCs). Relevant cellular and molecular mechanism(s) controlled by DEK in HNSCC remain poorly understood. While DEK is known to regulate specific transcriptional targets, global DEK-dependent gene networks in HNSCC are unknown. To identify DEK transcriptional signatures we performed RNA-Sequencing (RNA-Seq) in HNSCC cell lines that were either proficient or deficient for DEK. Bioinformatic analyses and subsequent validation revealed that IRAK1, a regulator of inflammatory signaling, and IRAK1-dependent regulatory networks were significantly repressed upon DEK knockdown in HNSCC. According to TCGA data, 14% of HNSCC specimens overexpressed IRAK1, thus supporting possible oncogenic functions. Furthermore, genetic or pharmacologic inhibition of IRAK1 in HNSCC cell lines was sufficient to attenuate downstream signaling such as ERK1/2 and to induce HNSCC cell death by apoptosis. Finally, targeting DEK and IRAK1 simultaneously enhanced cell death as compared to targeting either alone. Our findings reveal that IRAK1 promotes cell survival and is an attractive therapeutic target in HNSCC cells. Thus, we propose a model wherein IRAK1 stimulates tumor signaling and phenotypes both independently and in conjunction with DEK.
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spelling pubmed-47912392016-03-28 IRAK1 is a novel DEK transcriptional target and is essential for head and neck cancer cell survival Adams, Allie K. Bolanos, Lyndsey C. Dexheimer, Phillip J. Karns, Rebekah A. Aronow, Bruce J. Komurov, Kakajan Jegga, Anil G. Casper, Keith A. Patil, Yash J. Wilson, Keith M. Starczynowski, Daniel T. Wells, Susanne I. Oncotarget Research Paper The chromatin-binding DEK protein was recently reported to promote the growth of HPV(+) and HPV(−) head and neck squamous cell carcinomas (HNSCCs). Relevant cellular and molecular mechanism(s) controlled by DEK in HNSCC remain poorly understood. While DEK is known to regulate specific transcriptional targets, global DEK-dependent gene networks in HNSCC are unknown. To identify DEK transcriptional signatures we performed RNA-Sequencing (RNA-Seq) in HNSCC cell lines that were either proficient or deficient for DEK. Bioinformatic analyses and subsequent validation revealed that IRAK1, a regulator of inflammatory signaling, and IRAK1-dependent regulatory networks were significantly repressed upon DEK knockdown in HNSCC. According to TCGA data, 14% of HNSCC specimens overexpressed IRAK1, thus supporting possible oncogenic functions. Furthermore, genetic or pharmacologic inhibition of IRAK1 in HNSCC cell lines was sufficient to attenuate downstream signaling such as ERK1/2 and to induce HNSCC cell death by apoptosis. Finally, targeting DEK and IRAK1 simultaneously enhanced cell death as compared to targeting either alone. Our findings reveal that IRAK1 promotes cell survival and is an attractive therapeutic target in HNSCC cells. Thus, we propose a model wherein IRAK1 stimulates tumor signaling and phenotypes both independently and in conjunction with DEK. Impact Journals LLC 2015-10-26 /pmc/articles/PMC4791239/ /pubmed/26527316 Text en Copyright: © 2015 Adams et al. http://creativecommons.org/licenses/by/2.5/ 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 credited.
spellingShingle Research Paper
Adams, Allie K.
Bolanos, Lyndsey C.
Dexheimer, Phillip J.
Karns, Rebekah A.
Aronow, Bruce J.
Komurov, Kakajan
Jegga, Anil G.
Casper, Keith A.
Patil, Yash J.
Wilson, Keith M.
Starczynowski, Daniel T.
Wells, Susanne I.
IRAK1 is a novel DEK transcriptional target and is essential for head and neck cancer cell survival
title IRAK1 is a novel DEK transcriptional target and is essential for head and neck cancer cell survival
title_full IRAK1 is a novel DEK transcriptional target and is essential for head and neck cancer cell survival
title_fullStr IRAK1 is a novel DEK transcriptional target and is essential for head and neck cancer cell survival
title_full_unstemmed IRAK1 is a novel DEK transcriptional target and is essential for head and neck cancer cell survival
title_short IRAK1 is a novel DEK transcriptional target and is essential for head and neck cancer cell survival
title_sort irak1 is a novel dek transcriptional target and is essential for head and neck cancer cell survival
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4791239/
https://www.ncbi.nlm.nih.gov/pubmed/26527316
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