Selective CDK9 Inhibition by Natural Compound Toyocamycin in Cancer Cells

SIMPLE SUMMARY: By combining drug screens, transcriptomic studies, and in vitro assays, our study identified the natural product toyocamycin as a potent and selective CDK9 inhibitor. Thus, toyocamycin can be used as a new small molecule to modulate CDK9 activity in preclinical research. Through dock...

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Autores principales: Pandey, Somnath, Djibo, Rahinatou, Darracq, Anaïs, Calendo, Gennaro, Zhang, Hanghang, Henry, Ryan A., Andrews, Andrew J., Baylin, Stephen B., Madzo, Jozef, Najmanovich, Rafael, Issa, Jean-Pierre J., Raynal, Noël J.-M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9324262/
https://www.ncbi.nlm.nih.gov/pubmed/35884401
http://dx.doi.org/10.3390/cancers14143340
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author Pandey, Somnath
Djibo, Rahinatou
Darracq, Anaïs
Calendo, Gennaro
Zhang, Hanghang
Henry, Ryan A.
Andrews, Andrew J.
Baylin, Stephen B.
Madzo, Jozef
Najmanovich, Rafael
Issa, Jean-Pierre J.
Raynal, Noël J.-M.
author_facet Pandey, Somnath
Djibo, Rahinatou
Darracq, Anaïs
Calendo, Gennaro
Zhang, Hanghang
Henry, Ryan A.
Andrews, Andrew J.
Baylin, Stephen B.
Madzo, Jozef
Najmanovich, Rafael
Issa, Jean-Pierre J.
Raynal, Noël J.-M.
author_sort Pandey, Somnath
collection PubMed
description SIMPLE SUMMARY: By combining drug screens, transcriptomic studies, and in vitro assays, our study identified the natural product toyocamycin as a potent and selective CDK9 inhibitor. Thus, toyocamycin can be used as a new small molecule to modulate CDK9 activity in preclinical research. Through docking simulations, we identified its specific binding sites, which could spark some interest to design novel small molecule CDK9 inhibitors. ABSTRACT: Aberrant transcription in cancer cells involves the silencing of tumor suppressor genes (TSGs) and activation of oncogenes. Transcriptomic changes are associated with epigenomic alterations such as DNA-hypermethylation, histone deacetylation, and chromatin condensation in promoter regions of silenced TSGs. To discover novel drugs that trigger TSG reactivation in cancer cells, we used a GFP-reporter system whose expression is silenced by promoter DNA hypermethylation and histone deacetylation. After screening a natural product drug library, we identified that toyocamycin, an adenosine-analog, induces potent GFP reactivation and loss of clonogenicity in human colon cancer cells. Connectivity-mapping analysis revealed that toyocamycin produces a pharmacological signature mimicking cyclin-dependent kinase (CDK) inhibitors. RNA-sequencing revealed that the toyocamycin transcriptomic signature resembles that of a specific CDK9 inhibitor (HH1). Specific inhibition of RNA Pol II phosphorylation level and kinase assays confirmed that toyocamycin specifically inhibits CDK9 (IC(50) = 79 nM) with a greater efficacy than other CDKs (IC(50) values between 0.67 and 15 µM). Molecular docking showed that toyocamycin efficiently binds the CDK9 catalytic site in a conformation that differs from other CDKs, explained by the binding contribution of specific amino acids within the catalytic pocket and protein backbone. Altogether, we demonstrated that toyocamycin exhibits specific CDK9 inhibition in cancer cells, highlighting its potential for cancer chemotherapy.
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spelling pubmed-93242622022-07-27 Selective CDK9 Inhibition by Natural Compound Toyocamycin in Cancer Cells Pandey, Somnath Djibo, Rahinatou Darracq, Anaïs Calendo, Gennaro Zhang, Hanghang Henry, Ryan A. Andrews, Andrew J. Baylin, Stephen B. Madzo, Jozef Najmanovich, Rafael Issa, Jean-Pierre J. Raynal, Noël J.-M. Cancers (Basel) Article SIMPLE SUMMARY: By combining drug screens, transcriptomic studies, and in vitro assays, our study identified the natural product toyocamycin as a potent and selective CDK9 inhibitor. Thus, toyocamycin can be used as a new small molecule to modulate CDK9 activity in preclinical research. Through docking simulations, we identified its specific binding sites, which could spark some interest to design novel small molecule CDK9 inhibitors. ABSTRACT: Aberrant transcription in cancer cells involves the silencing of tumor suppressor genes (TSGs) and activation of oncogenes. Transcriptomic changes are associated with epigenomic alterations such as DNA-hypermethylation, histone deacetylation, and chromatin condensation in promoter regions of silenced TSGs. To discover novel drugs that trigger TSG reactivation in cancer cells, we used a GFP-reporter system whose expression is silenced by promoter DNA hypermethylation and histone deacetylation. After screening a natural product drug library, we identified that toyocamycin, an adenosine-analog, induces potent GFP reactivation and loss of clonogenicity in human colon cancer cells. Connectivity-mapping analysis revealed that toyocamycin produces a pharmacological signature mimicking cyclin-dependent kinase (CDK) inhibitors. RNA-sequencing revealed that the toyocamycin transcriptomic signature resembles that of a specific CDK9 inhibitor (HH1). Specific inhibition of RNA Pol II phosphorylation level and kinase assays confirmed that toyocamycin specifically inhibits CDK9 (IC(50) = 79 nM) with a greater efficacy than other CDKs (IC(50) values between 0.67 and 15 µM). Molecular docking showed that toyocamycin efficiently binds the CDK9 catalytic site in a conformation that differs from other CDKs, explained by the binding contribution of specific amino acids within the catalytic pocket and protein backbone. Altogether, we demonstrated that toyocamycin exhibits specific CDK9 inhibition in cancer cells, highlighting its potential for cancer chemotherapy. MDPI 2022-07-08 /pmc/articles/PMC9324262/ /pubmed/35884401 http://dx.doi.org/10.3390/cancers14143340 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Pandey, Somnath
Djibo, Rahinatou
Darracq, Anaïs
Calendo, Gennaro
Zhang, Hanghang
Henry, Ryan A.
Andrews, Andrew J.
Baylin, Stephen B.
Madzo, Jozef
Najmanovich, Rafael
Issa, Jean-Pierre J.
Raynal, Noël J.-M.
Selective CDK9 Inhibition by Natural Compound Toyocamycin in Cancer Cells
title Selective CDK9 Inhibition by Natural Compound Toyocamycin in Cancer Cells
title_full Selective CDK9 Inhibition by Natural Compound Toyocamycin in Cancer Cells
title_fullStr Selective CDK9 Inhibition by Natural Compound Toyocamycin in Cancer Cells
title_full_unstemmed Selective CDK9 Inhibition by Natural Compound Toyocamycin in Cancer Cells
title_short Selective CDK9 Inhibition by Natural Compound Toyocamycin in Cancer Cells
title_sort selective cdk9 inhibition by natural compound toyocamycin in cancer cells
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9324262/
https://www.ncbi.nlm.nih.gov/pubmed/35884401
http://dx.doi.org/10.3390/cancers14143340
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