A Computational Approach with Biological Evaluation: Combinatorial Treatment of Curcumin and Exemestane Synergistically Regulates DDX3 Expression in Cancer Cell Lines

DDX3 belongs to RNA helicase family that demonstrates oncogenic properties and has gained wider attention due to its role in cancer progression, proliferation and transformation. Mounting reports have evidenced the role of DDX3 in cancers making it a promising target to abrogate DDX3 triggered cance...

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Autores principales: Rampogu, Shailima, Kim, Seong Min, Son, Minky, Baek, Ayoung, Park, Chanin, Lee, Gihwan, Kim, Yumi, Kim, Gon Sup, Kim, Ju Hyun, Lee, Keun Woo
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7355417/
https://www.ncbi.nlm.nih.gov/pubmed/32512851
http://dx.doi.org/10.3390/biom10060857
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author Rampogu, Shailima
Kim, Seong Min
Son, Minky
Baek, Ayoung
Park, Chanin
Lee, Gihwan
Kim, Yumi
Kim, Gon Sup
Kim, Ju Hyun
Lee, Keun Woo
author_facet Rampogu, Shailima
Kim, Seong Min
Son, Minky
Baek, Ayoung
Park, Chanin
Lee, Gihwan
Kim, Yumi
Kim, Gon Sup
Kim, Ju Hyun
Lee, Keun Woo
author_sort Rampogu, Shailima
collection PubMed
description DDX3 belongs to RNA helicase family that demonstrates oncogenic properties and has gained wider attention due to its role in cancer progression, proliferation and transformation. Mounting reports have evidenced the role of DDX3 in cancers making it a promising target to abrogate DDX3 triggered cancers. Dual pharmacophore models were generated and were subsequently validated. They were used as 3D queries to screen the InterBioScreen database, resulting in the selection of curcumin that was escalated to molecular dynamics simulation studies. In vitro anti-cancer analysis was conducted on three cell lines such as MCF-7, MDA-MB-231 and HeLa, which were evaluated along with exemestane. Curcumin was docked into the active site of the protein target (PDB code 2I4I) to estimate the binding affinity. The compound has interacted with two key residues and has displayed stable molecular dynamics simulation results. In vitro analysis has demonstrated that both the candidate compounds have reduced the expression of DDX3 in three cell lines. However, upon combinatorial treatment of curcumin (10 and 20 μM) and exemestane (50 μM) a synergism was exhibited, strikingly downregulating the DDX3 expression and has enhanced apoptosis in three cell lines. The obtained results illuminate the use of curcumin as an alternative DDX3 inhibitor and can serve as a chemical scaffold to design new small molecules.
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spelling pubmed-73554172020-07-23 A Computational Approach with Biological Evaluation: Combinatorial Treatment of Curcumin and Exemestane Synergistically Regulates DDX3 Expression in Cancer Cell Lines Rampogu, Shailima Kim, Seong Min Son, Minky Baek, Ayoung Park, Chanin Lee, Gihwan Kim, Yumi Kim, Gon Sup Kim, Ju Hyun Lee, Keun Woo Biomolecules Article DDX3 belongs to RNA helicase family that demonstrates oncogenic properties and has gained wider attention due to its role in cancer progression, proliferation and transformation. Mounting reports have evidenced the role of DDX3 in cancers making it a promising target to abrogate DDX3 triggered cancers. Dual pharmacophore models were generated and were subsequently validated. They were used as 3D queries to screen the InterBioScreen database, resulting in the selection of curcumin that was escalated to molecular dynamics simulation studies. In vitro anti-cancer analysis was conducted on three cell lines such as MCF-7, MDA-MB-231 and HeLa, which were evaluated along with exemestane. Curcumin was docked into the active site of the protein target (PDB code 2I4I) to estimate the binding affinity. The compound has interacted with two key residues and has displayed stable molecular dynamics simulation results. In vitro analysis has demonstrated that both the candidate compounds have reduced the expression of DDX3 in three cell lines. However, upon combinatorial treatment of curcumin (10 and 20 μM) and exemestane (50 μM) a synergism was exhibited, strikingly downregulating the DDX3 expression and has enhanced apoptosis in three cell lines. The obtained results illuminate the use of curcumin as an alternative DDX3 inhibitor and can serve as a chemical scaffold to design new small molecules. MDPI 2020-06-04 /pmc/articles/PMC7355417/ /pubmed/32512851 http://dx.doi.org/10.3390/biom10060857 Text en © 2020 by the authors. 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 (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Rampogu, Shailima
Kim, Seong Min
Son, Minky
Baek, Ayoung
Park, Chanin
Lee, Gihwan
Kim, Yumi
Kim, Gon Sup
Kim, Ju Hyun
Lee, Keun Woo
A Computational Approach with Biological Evaluation: Combinatorial Treatment of Curcumin and Exemestane Synergistically Regulates DDX3 Expression in Cancer Cell Lines
title A Computational Approach with Biological Evaluation: Combinatorial Treatment of Curcumin and Exemestane Synergistically Regulates DDX3 Expression in Cancer Cell Lines
title_full A Computational Approach with Biological Evaluation: Combinatorial Treatment of Curcumin and Exemestane Synergistically Regulates DDX3 Expression in Cancer Cell Lines
title_fullStr A Computational Approach with Biological Evaluation: Combinatorial Treatment of Curcumin and Exemestane Synergistically Regulates DDX3 Expression in Cancer Cell Lines
title_full_unstemmed A Computational Approach with Biological Evaluation: Combinatorial Treatment of Curcumin and Exemestane Synergistically Regulates DDX3 Expression in Cancer Cell Lines
title_short A Computational Approach with Biological Evaluation: Combinatorial Treatment of Curcumin and Exemestane Synergistically Regulates DDX3 Expression in Cancer Cell Lines
title_sort computational approach with biological evaluation: combinatorial treatment of curcumin and exemestane synergistically regulates ddx3 expression in cancer cell lines
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7355417/
https://www.ncbi.nlm.nih.gov/pubmed/32512851
http://dx.doi.org/10.3390/biom10060857
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