Reactivation of ERK and Akt confers resistance of mutant BRAF colon cancer cells to the HSP90 inhibitor AUY922

Oncogenic mutations of BRAF occur in approximately 10% of colon cancers and are associated with their resistance to clinically available therapeutic drugs and poor prognosis of the patients. Here we report that colon cancer cells with mutant BRAF are also resistant to the heat shock protein 90 (HSP9...

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Autores principales: Wang, Chun Yan, Guo, Su Tang, Wang, Jia Yu, Yan, Xu Guang, Farrelly, Margaret, Zhang, Yuan Yuan, Liu, Fen, Yari, Hamed, La, Ting, Lei, Fu Xi, Jin, Lei, Zhang, Xu Dong, Jiang, Chen Chen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5226532/
https://www.ncbi.nlm.nih.gov/pubmed/27391062
http://dx.doi.org/10.18632/oncotarget.10414
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author Wang, Chun Yan
Guo, Su Tang
Wang, Jia Yu
Yan, Xu Guang
Farrelly, Margaret
Zhang, Yuan Yuan
Liu, Fen
Yari, Hamed
La, Ting
Lei, Fu Xi
Jin, Lei
Zhang, Xu Dong
Jiang, Chen Chen
author_facet Wang, Chun Yan
Guo, Su Tang
Wang, Jia Yu
Yan, Xu Guang
Farrelly, Margaret
Zhang, Yuan Yuan
Liu, Fen
Yari, Hamed
La, Ting
Lei, Fu Xi
Jin, Lei
Zhang, Xu Dong
Jiang, Chen Chen
author_sort Wang, Chun Yan
collection PubMed
description Oncogenic mutations of BRAF occur in approximately 10% of colon cancers and are associated with their resistance to clinically available therapeutic drugs and poor prognosis of the patients. Here we report that colon cancer cells with mutant BRAF are also resistant to the heat shock protein 90 (HSP90) inhibitor AUY922, and that this is caused by rebound activation of ERK and Akt. Although AUY922 triggered rapid reduction in ERK and Akt activation in both wild-type and mutant BRAF colon cancer cells, activation of ERK and Akt rebounded shortly in the latter leading to resistance of the cells to AUY922-induced apoptosis. Reactivation of ERK was associated with the persistent expression of mutant BRAF, which, despite being a client of HSP90, was only partially degraded by AUY922, whereas reactivation of Akt was related to the activity of the HSP90 co-chaperone, cell division cycle 37 (CDC37), in that knockdown of CDC37 inhibited Akt reactivation in mutant colon cancer cells treated with AUY922. In support, as a HSP90 client protein, Akt was only diminished by AUY922 in wild-type but not mutant BRAF colon cancer cells. Collectively, these results reveal that reactivation of ERK and Akt associated respectively with the activity of mutant BRAF and CDC37 renders mutant BRAF colon cancer cells resistant to AUY922, with implications of co-targeting mutant BRAF and/or CDC37 and HSP90 in the treatment of mutant BRAF colon cancers.
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spelling pubmed-52265322017-01-18 Reactivation of ERK and Akt confers resistance of mutant BRAF colon cancer cells to the HSP90 inhibitor AUY922 Wang, Chun Yan Guo, Su Tang Wang, Jia Yu Yan, Xu Guang Farrelly, Margaret Zhang, Yuan Yuan Liu, Fen Yari, Hamed La, Ting Lei, Fu Xi Jin, Lei Zhang, Xu Dong Jiang, Chen Chen Oncotarget Research Paper Oncogenic mutations of BRAF occur in approximately 10% of colon cancers and are associated with their resistance to clinically available therapeutic drugs and poor prognosis of the patients. Here we report that colon cancer cells with mutant BRAF are also resistant to the heat shock protein 90 (HSP90) inhibitor AUY922, and that this is caused by rebound activation of ERK and Akt. Although AUY922 triggered rapid reduction in ERK and Akt activation in both wild-type and mutant BRAF colon cancer cells, activation of ERK and Akt rebounded shortly in the latter leading to resistance of the cells to AUY922-induced apoptosis. Reactivation of ERK was associated with the persistent expression of mutant BRAF, which, despite being a client of HSP90, was only partially degraded by AUY922, whereas reactivation of Akt was related to the activity of the HSP90 co-chaperone, cell division cycle 37 (CDC37), in that knockdown of CDC37 inhibited Akt reactivation in mutant colon cancer cells treated with AUY922. In support, as a HSP90 client protein, Akt was only diminished by AUY922 in wild-type but not mutant BRAF colon cancer cells. Collectively, these results reveal that reactivation of ERK and Akt associated respectively with the activity of mutant BRAF and CDC37 renders mutant BRAF colon cancer cells resistant to AUY922, with implications of co-targeting mutant BRAF and/or CDC37 and HSP90 in the treatment of mutant BRAF colon cancers. Impact Journals LLC 2016-07-06 /pmc/articles/PMC5226532/ /pubmed/27391062 http://dx.doi.org/10.18632/oncotarget.10414 Text en Copyright: © 2016 Wang 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
Wang, Chun Yan
Guo, Su Tang
Wang, Jia Yu
Yan, Xu Guang
Farrelly, Margaret
Zhang, Yuan Yuan
Liu, Fen
Yari, Hamed
La, Ting
Lei, Fu Xi
Jin, Lei
Zhang, Xu Dong
Jiang, Chen Chen
Reactivation of ERK and Akt confers resistance of mutant BRAF colon cancer cells to the HSP90 inhibitor AUY922
title Reactivation of ERK and Akt confers resistance of mutant BRAF colon cancer cells to the HSP90 inhibitor AUY922
title_full Reactivation of ERK and Akt confers resistance of mutant BRAF colon cancer cells to the HSP90 inhibitor AUY922
title_fullStr Reactivation of ERK and Akt confers resistance of mutant BRAF colon cancer cells to the HSP90 inhibitor AUY922
title_full_unstemmed Reactivation of ERK and Akt confers resistance of mutant BRAF colon cancer cells to the HSP90 inhibitor AUY922
title_short Reactivation of ERK and Akt confers resistance of mutant BRAF colon cancer cells to the HSP90 inhibitor AUY922
title_sort reactivation of erk and akt confers resistance of mutant braf colon cancer cells to the hsp90 inhibitor auy922
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5226532/
https://www.ncbi.nlm.nih.gov/pubmed/27391062
http://dx.doi.org/10.18632/oncotarget.10414
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