Kinome inhibition reveals a role for polo‐like kinase 1 in targeting post‐transcriptional control in cancer

Dysfunctions in post‐transcriptional control are observed in cancer and chronic inflammatory diseases. Here, we employed a kinome inhibitor library (n = 378) in a reporter system selective for 3′‐untranslated region–AU‐rich elements (ARE). Fifteen inhibitors reduced the ARE‐reporter activity; among...

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Autores principales: Al‐Qahtani, Qamraa H., Moghrabi, Walid N., Al‐Yahya, Suhad, Al‐Haj, Latifa, Al‐Saif, Maher, Mahmoud, Linah, Al‐Mohanna, Falah, Al‐Souhibani, Norah, Alaiya, Ayodele, Hitti, Edward, Khabar, Khalid S. A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2021
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8334256/
https://www.ncbi.nlm.nih.gov/pubmed/33411958
http://dx.doi.org/10.1002/1878-0261.12897
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author Al‐Qahtani, Qamraa H.
Moghrabi, Walid N.
Al‐Yahya, Suhad
Al‐Haj, Latifa
Al‐Saif, Maher
Mahmoud, Linah
Al‐Mohanna, Falah
Al‐Souhibani, Norah
Alaiya, Ayodele
Hitti, Edward
Khabar, Khalid S. A.
author_facet Al‐Qahtani, Qamraa H.
Moghrabi, Walid N.
Al‐Yahya, Suhad
Al‐Haj, Latifa
Al‐Saif, Maher
Mahmoud, Linah
Al‐Mohanna, Falah
Al‐Souhibani, Norah
Alaiya, Ayodele
Hitti, Edward
Khabar, Khalid S. A.
author_sort Al‐Qahtani, Qamraa H.
collection PubMed
description Dysfunctions in post‐transcriptional control are observed in cancer and chronic inflammatory diseases. Here, we employed a kinome inhibitor library (n = 378) in a reporter system selective for 3′‐untranslated region–AU‐rich elements (ARE). Fifteen inhibitors reduced the ARE‐reporter activity; among the targets is the polo‐like kinase 1 (PLK1). RNA‐seq experiments demonstrated that the PLK1 inhibitor, volasertib, reduces the expression of cytokine and cell growth ARE mRNAs. PLK1 inhibition caused accelerated mRNA decay in cancer cells and was associated with reduced phosphorylation and stability of the mRNA decay‐promoting protein, tristetraprolin (ZFP36/TTP). Ectopic expression of PLK1 increased abundance and stability of high molecular weight of ZFP36/TTP likely of the phosphorylated form. PLK1 effect was associated with the MAPK‐MK2 pathway, a major regulator of ARE‐mRNA stability, as evident from MK2 inhibition, in vitro phosphorylation, and knockout experiments. Mutational analysis demonstrates that TTP serine 186 is a target for PLK1 effect. Treatment of mice with the PLK1 inhibitor reduced both ZFP36/TTP phosphorylation in xenograft tumor tissues, and the tumor size. In cancer patients' tissues, PLK1/ARE‐regulated gene cluster was overexpressed in solid tumors and associated with poor survival. The data showed that PLK1‐mediated post‐transcriptional aberration could be a therapeutic target.
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spelling pubmed-83342562021-08-09 Kinome inhibition reveals a role for polo‐like kinase 1 in targeting post‐transcriptional control in cancer Al‐Qahtani, Qamraa H. Moghrabi, Walid N. Al‐Yahya, Suhad Al‐Haj, Latifa Al‐Saif, Maher Mahmoud, Linah Al‐Mohanna, Falah Al‐Souhibani, Norah Alaiya, Ayodele Hitti, Edward Khabar, Khalid S. A. Mol Oncol Research Articles Dysfunctions in post‐transcriptional control are observed in cancer and chronic inflammatory diseases. Here, we employed a kinome inhibitor library (n = 378) in a reporter system selective for 3′‐untranslated region–AU‐rich elements (ARE). Fifteen inhibitors reduced the ARE‐reporter activity; among the targets is the polo‐like kinase 1 (PLK1). RNA‐seq experiments demonstrated that the PLK1 inhibitor, volasertib, reduces the expression of cytokine and cell growth ARE mRNAs. PLK1 inhibition caused accelerated mRNA decay in cancer cells and was associated with reduced phosphorylation and stability of the mRNA decay‐promoting protein, tristetraprolin (ZFP36/TTP). Ectopic expression of PLK1 increased abundance and stability of high molecular weight of ZFP36/TTP likely of the phosphorylated form. PLK1 effect was associated with the MAPK‐MK2 pathway, a major regulator of ARE‐mRNA stability, as evident from MK2 inhibition, in vitro phosphorylation, and knockout experiments. Mutational analysis demonstrates that TTP serine 186 is a target for PLK1 effect. Treatment of mice with the PLK1 inhibitor reduced both ZFP36/TTP phosphorylation in xenograft tumor tissues, and the tumor size. In cancer patients' tissues, PLK1/ARE‐regulated gene cluster was overexpressed in solid tumors and associated with poor survival. The data showed that PLK1‐mediated post‐transcriptional aberration could be a therapeutic target. John Wiley and Sons Inc. 2021-02-01 2021-08 /pmc/articles/PMC8334256/ /pubmed/33411958 http://dx.doi.org/10.1002/1878-0261.12897 Text en © 2021 The Authors. Molecular Oncology published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
Al‐Qahtani, Qamraa H.
Moghrabi, Walid N.
Al‐Yahya, Suhad
Al‐Haj, Latifa
Al‐Saif, Maher
Mahmoud, Linah
Al‐Mohanna, Falah
Al‐Souhibani, Norah
Alaiya, Ayodele
Hitti, Edward
Khabar, Khalid S. A.
Kinome inhibition reveals a role for polo‐like kinase 1 in targeting post‐transcriptional control in cancer
title Kinome inhibition reveals a role for polo‐like kinase 1 in targeting post‐transcriptional control in cancer
title_full Kinome inhibition reveals a role for polo‐like kinase 1 in targeting post‐transcriptional control in cancer
title_fullStr Kinome inhibition reveals a role for polo‐like kinase 1 in targeting post‐transcriptional control in cancer
title_full_unstemmed Kinome inhibition reveals a role for polo‐like kinase 1 in targeting post‐transcriptional control in cancer
title_short Kinome inhibition reveals a role for polo‐like kinase 1 in targeting post‐transcriptional control in cancer
title_sort kinome inhibition reveals a role for polo‐like kinase 1 in targeting post‐transcriptional control in cancer
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8334256/
https://www.ncbi.nlm.nih.gov/pubmed/33411958
http://dx.doi.org/10.1002/1878-0261.12897
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