Cytotoxic Activity, Topoisomerase I Inhibition and In Silico Studies of New Sesquiterpene-aryl Ester Derivatives of (-) Drimenol

In this study, we aimed to evaluate two sets of sesquiterpene-aryl derivatives linked by an ester bond, their cytotoxic activities, and their capacity to activate caspases 3/7 and inhibit human topoisomerase I (TOP1). A total of 13 compounds were synthesized from the natural sesquiterpene (-)-drimen...

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Autores principales: Araque, Ileana, Ramírez, Javiera, Vergara, Rut, Mella, Jaime, Aránguiz, Pablo, Espinoza, Luis, Vera, Waleska, Montenegro, Iván, Salas, Cristian O., Villena, Joan, Cuellar, Mauricio A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10179937/
https://www.ncbi.nlm.nih.gov/pubmed/37175368
http://dx.doi.org/10.3390/molecules28093959
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author Araque, Ileana
Ramírez, Javiera
Vergara, Rut
Mella, Jaime
Aránguiz, Pablo
Espinoza, Luis
Vera, Waleska
Montenegro, Iván
Salas, Cristian O.
Villena, Joan
Cuellar, Mauricio A.
author_facet Araque, Ileana
Ramírez, Javiera
Vergara, Rut
Mella, Jaime
Aránguiz, Pablo
Espinoza, Luis
Vera, Waleska
Montenegro, Iván
Salas, Cristian O.
Villena, Joan
Cuellar, Mauricio A.
author_sort Araque, Ileana
collection PubMed
description In this study, we aimed to evaluate two sets of sesquiterpene-aryl derivatives linked by an ester bond, their cytotoxic activities, and their capacity to activate caspases 3/7 and inhibit human topoisomerase I (TOP1). A total of 13 compounds were synthesized from the natural sesquiterpene (-)-drimenol and their cytotoxic activity was evaluated in vitro against three cancer cell lines: PC-3 (prostate cancer), HT-29 (colon cancer), MCF-7 (breast cancer), and an immortalized non-tumoral cell line (MCF-10). From the results, it was observed that 6a was the most promising compound due to its cytotoxic effect on three cancer cell lines and its selectivity, 6a was 100-fold more selective than 5-FU in MCF-7 and 20-fold in PC-3. It was observed that 6a also induced apoptosis by caspases 3/7 activity using a Capsase-Glo-3/7 assay kit and inhibited TOP1. A possible binding mode of 6a in a complex with TOP1-DNA was proposed by docking and molecular dynamics studies. In addition, 6a was predicted to have a good pharmacokinetic profile for oral administration. Therefore, through this study, it was demonstrated that the drimane scaffold should be considered in the search of new antitumoral agents.
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spelling pubmed-101799372023-05-13 Cytotoxic Activity, Topoisomerase I Inhibition and In Silico Studies of New Sesquiterpene-aryl Ester Derivatives of (-) Drimenol Araque, Ileana Ramírez, Javiera Vergara, Rut Mella, Jaime Aránguiz, Pablo Espinoza, Luis Vera, Waleska Montenegro, Iván Salas, Cristian O. Villena, Joan Cuellar, Mauricio A. Molecules Article In this study, we aimed to evaluate two sets of sesquiterpene-aryl derivatives linked by an ester bond, their cytotoxic activities, and their capacity to activate caspases 3/7 and inhibit human topoisomerase I (TOP1). A total of 13 compounds were synthesized from the natural sesquiterpene (-)-drimenol and their cytotoxic activity was evaluated in vitro against three cancer cell lines: PC-3 (prostate cancer), HT-29 (colon cancer), MCF-7 (breast cancer), and an immortalized non-tumoral cell line (MCF-10). From the results, it was observed that 6a was the most promising compound due to its cytotoxic effect on three cancer cell lines and its selectivity, 6a was 100-fold more selective than 5-FU in MCF-7 and 20-fold in PC-3. It was observed that 6a also induced apoptosis by caspases 3/7 activity using a Capsase-Glo-3/7 assay kit and inhibited TOP1. A possible binding mode of 6a in a complex with TOP1-DNA was proposed by docking and molecular dynamics studies. In addition, 6a was predicted to have a good pharmacokinetic profile for oral administration. Therefore, through this study, it was demonstrated that the drimane scaffold should be considered in the search of new antitumoral agents. MDPI 2023-05-08 /pmc/articles/PMC10179937/ /pubmed/37175368 http://dx.doi.org/10.3390/molecules28093959 Text en © 2023 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
Araque, Ileana
Ramírez, Javiera
Vergara, Rut
Mella, Jaime
Aránguiz, Pablo
Espinoza, Luis
Vera, Waleska
Montenegro, Iván
Salas, Cristian O.
Villena, Joan
Cuellar, Mauricio A.
Cytotoxic Activity, Topoisomerase I Inhibition and In Silico Studies of New Sesquiterpene-aryl Ester Derivatives of (-) Drimenol
title Cytotoxic Activity, Topoisomerase I Inhibition and In Silico Studies of New Sesquiterpene-aryl Ester Derivatives of (-) Drimenol
title_full Cytotoxic Activity, Topoisomerase I Inhibition and In Silico Studies of New Sesquiterpene-aryl Ester Derivatives of (-) Drimenol
title_fullStr Cytotoxic Activity, Topoisomerase I Inhibition and In Silico Studies of New Sesquiterpene-aryl Ester Derivatives of (-) Drimenol
title_full_unstemmed Cytotoxic Activity, Topoisomerase I Inhibition and In Silico Studies of New Sesquiterpene-aryl Ester Derivatives of (-) Drimenol
title_short Cytotoxic Activity, Topoisomerase I Inhibition and In Silico Studies of New Sesquiterpene-aryl Ester Derivatives of (-) Drimenol
title_sort cytotoxic activity, topoisomerase i inhibition and in silico studies of new sesquiterpene-aryl ester derivatives of (-) drimenol
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10179937/
https://www.ncbi.nlm.nih.gov/pubmed/37175368
http://dx.doi.org/10.3390/molecules28093959
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