Targeting BRF2 in Cancer Using Repurposed Drugs

SIMPLE SUMMARY: BRF2, a subunit of the RNA polymerase III transcription complex, is upregulated in a wide variety of cancers and is a potential therapeutic target; however, no effective drugs are available to target BRF2. The upregulation of BRF2 in cancer cells confers survival via the prevention o...

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Autores principales: Rashidieh, Behnam, Molakarimi, Maryam, Mohseni, Ammar, Tria, Simon Manuel, Truong, Hein, Srihari, Sriganesh, Adams, Rachael C., Jones, Mathew, Duijf, Pascal H. G., Kalimutho, Murugan, Khanna, Kum Kum
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8345145/
https://www.ncbi.nlm.nih.gov/pubmed/34359683
http://dx.doi.org/10.3390/cancers13153778
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author Rashidieh, Behnam
Molakarimi, Maryam
Mohseni, Ammar
Tria, Simon Manuel
Truong, Hein
Srihari, Sriganesh
Adams, Rachael C.
Jones, Mathew
Duijf, Pascal H. G.
Kalimutho, Murugan
Khanna, Kum Kum
author_facet Rashidieh, Behnam
Molakarimi, Maryam
Mohseni, Ammar
Tria, Simon Manuel
Truong, Hein
Srihari, Sriganesh
Adams, Rachael C.
Jones, Mathew
Duijf, Pascal H. G.
Kalimutho, Murugan
Khanna, Kum Kum
author_sort Rashidieh, Behnam
collection PubMed
description SIMPLE SUMMARY: BRF2, a subunit of the RNA polymerase III transcription complex, is upregulated in a wide variety of cancers and is a potential therapeutic target; however, no effective drugs are available to target BRF2. The upregulation of BRF2 in cancer cells confers survival via the prevention of oxidative stress-induced apoptosis. In this manuscript, we report the identification of potential BRF2 inhibitors through in silico drug repurposing screening. We further characterized bexarotene as a hit compound for the development of selective BRF2 inhibitors and provide experimental validation to support the repurposing of this FDA-approved drug as an agent to reduce the cellular levels of ROS and consequent BRF2 expression in cancers with elevated levels of oxidative stress. ABSTRACT: The overexpression of BRF2, a selective subunit of RNA polymerase III, has been shown to be crucial in the development of several types of cancers, including breast cancer and lung squamous cell carcinoma. Predominantly, BRF2 acts as a central redox-sensing transcription factor (TF) and is involved in rescuing oxidative stress (OS)-induced apoptosis. Here, we showed a novel link between BRF2 and the DNA damage response. Due to the lack of BRF2-specific inhibitors, through virtual screening and molecular dynamics simulation, we identified potential drug candidates that interfere with BRF2-TATA-binding Protein (TBP)-DNA complex interactions based on binding energy, intermolecular, and torsional energy parameters. We experimentally tested bexarotene as a potential BRF2 inhibitor. We found that bexarotene (Bex) treatment resulted in a dramatic decline in oxidative stress and Tert-butylhydroquinone (tBHQ)-induced levels of BRF2 and consequently led to a decrease in the cellular proliferation of cancer cells which may in part be due to the drug pretreatment-induced reduction of ROS generated by the oxidizing agent. Our data thus provide the first experimental evidence that BRF2 is a novel player in the DNA damage response pathway and that bexarotene can be used as a potential inhibitor to treat cancers with the specific elevation of oxidative stress.
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spelling pubmed-83451452021-08-07 Targeting BRF2 in Cancer Using Repurposed Drugs Rashidieh, Behnam Molakarimi, Maryam Mohseni, Ammar Tria, Simon Manuel Truong, Hein Srihari, Sriganesh Adams, Rachael C. Jones, Mathew Duijf, Pascal H. G. Kalimutho, Murugan Khanna, Kum Kum Cancers (Basel) Article SIMPLE SUMMARY: BRF2, a subunit of the RNA polymerase III transcription complex, is upregulated in a wide variety of cancers and is a potential therapeutic target; however, no effective drugs are available to target BRF2. The upregulation of BRF2 in cancer cells confers survival via the prevention of oxidative stress-induced apoptosis. In this manuscript, we report the identification of potential BRF2 inhibitors through in silico drug repurposing screening. We further characterized bexarotene as a hit compound for the development of selective BRF2 inhibitors and provide experimental validation to support the repurposing of this FDA-approved drug as an agent to reduce the cellular levels of ROS and consequent BRF2 expression in cancers with elevated levels of oxidative stress. ABSTRACT: The overexpression of BRF2, a selective subunit of RNA polymerase III, has been shown to be crucial in the development of several types of cancers, including breast cancer and lung squamous cell carcinoma. Predominantly, BRF2 acts as a central redox-sensing transcription factor (TF) and is involved in rescuing oxidative stress (OS)-induced apoptosis. Here, we showed a novel link between BRF2 and the DNA damage response. Due to the lack of BRF2-specific inhibitors, through virtual screening and molecular dynamics simulation, we identified potential drug candidates that interfere with BRF2-TATA-binding Protein (TBP)-DNA complex interactions based on binding energy, intermolecular, and torsional energy parameters. We experimentally tested bexarotene as a potential BRF2 inhibitor. We found that bexarotene (Bex) treatment resulted in a dramatic decline in oxidative stress and Tert-butylhydroquinone (tBHQ)-induced levels of BRF2 and consequently led to a decrease in the cellular proliferation of cancer cells which may in part be due to the drug pretreatment-induced reduction of ROS generated by the oxidizing agent. Our data thus provide the first experimental evidence that BRF2 is a novel player in the DNA damage response pathway and that bexarotene can be used as a potential inhibitor to treat cancers with the specific elevation of oxidative stress. MDPI 2021-07-27 /pmc/articles/PMC8345145/ /pubmed/34359683 http://dx.doi.org/10.3390/cancers13153778 Text en © 2021 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
Rashidieh, Behnam
Molakarimi, Maryam
Mohseni, Ammar
Tria, Simon Manuel
Truong, Hein
Srihari, Sriganesh
Adams, Rachael C.
Jones, Mathew
Duijf, Pascal H. G.
Kalimutho, Murugan
Khanna, Kum Kum
Targeting BRF2 in Cancer Using Repurposed Drugs
title Targeting BRF2 in Cancer Using Repurposed Drugs
title_full Targeting BRF2 in Cancer Using Repurposed Drugs
title_fullStr Targeting BRF2 in Cancer Using Repurposed Drugs
title_full_unstemmed Targeting BRF2 in Cancer Using Repurposed Drugs
title_short Targeting BRF2 in Cancer Using Repurposed Drugs
title_sort targeting brf2 in cancer using repurposed drugs
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8345145/
https://www.ncbi.nlm.nih.gov/pubmed/34359683
http://dx.doi.org/10.3390/cancers13153778
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