Sensitivity of Mitochondrial Transcription and Resistance of RNA Polymerase II Dependent Nuclear Transcription to Antiviral Ribonucleosides

Ribonucleoside analogues have potential utility as anti-viral, -parasitic, -bacterial and -cancer agents. However, their clinical applications have been limited by off target effects. Development of antiviral ribonucleosides for treatment of hepatitis C virus (HCV) infection has been hampered by app...

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Autores principales: Arnold, Jamie J., Sharma, Suresh D., Feng, Joy Y., Ray, Adrian S., Smidansky, Eric D., Kireeva, Maria L., Cho, Aesop, Perry, Jason, Vela, Jennifer E., Park, Yeojin, Xu, Yili, Tian, Yang, Babusis, Darius, Barauskus, Ona, Peterson, Blake R., Gnatt, Averell, Kashlev, Mikhail, Zhong, Weidong, Cameron, Craig E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3499576/
https://www.ncbi.nlm.nih.gov/pubmed/23166498
http://dx.doi.org/10.1371/journal.ppat.1003030
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author Arnold, Jamie J.
Sharma, Suresh D.
Feng, Joy Y.
Ray, Adrian S.
Smidansky, Eric D.
Kireeva, Maria L.
Cho, Aesop
Perry, Jason
Vela, Jennifer E.
Park, Yeojin
Xu, Yili
Tian, Yang
Babusis, Darius
Barauskus, Ona
Peterson, Blake R.
Gnatt, Averell
Kashlev, Mikhail
Zhong, Weidong
Cameron, Craig E.
author_facet Arnold, Jamie J.
Sharma, Suresh D.
Feng, Joy Y.
Ray, Adrian S.
Smidansky, Eric D.
Kireeva, Maria L.
Cho, Aesop
Perry, Jason
Vela, Jennifer E.
Park, Yeojin
Xu, Yili
Tian, Yang
Babusis, Darius
Barauskus, Ona
Peterson, Blake R.
Gnatt, Averell
Kashlev, Mikhail
Zhong, Weidong
Cameron, Craig E.
author_sort Arnold, Jamie J.
collection PubMed
description Ribonucleoside analogues have potential utility as anti-viral, -parasitic, -bacterial and -cancer agents. However, their clinical applications have been limited by off target effects. Development of antiviral ribonucleosides for treatment of hepatitis C virus (HCV) infection has been hampered by appearance of toxicity during clinical trials that evaded detection during preclinical studies. It is well established that the human mitochondrial DNA polymerase is an off target for deoxyribonucleoside reverse transcriptase inhibitors. Here we test the hypothesis that triphosphorylated metabolites of therapeutic ribonucleoside analogues are substrates for cellular RNA polymerases. We have used ribonucleoside analogues with activity against HCV as model compounds for therapeutic ribonucleosides. We have included ribonucleoside analogues containing 2′-C-methyl, 4′-methyl and 4′-azido substituents that are non-obligate chain terminators of the HCV RNA polymerase. We show that all of the anti-HCV ribonucleoside analogues are substrates for human mitochondrial RNA polymerase (POLRMT) and eukaryotic core RNA polymerase II (Pol II) in vitro. Unexpectedly, analogues containing 2′-C-methyl, 4′-methyl and 4′-azido substituents were inhibitors of POLRMT and Pol II. Importantly, the proofreading activity of TFIIS was capable of excising these analogues from Pol II transcripts. Evaluation of transcription in cells confirmed sensitivity of POLRMT to antiviral ribonucleosides, while Pol II remained predominantly refractory. We introduce a parameter termed the mitovir (mitochondrial dysfunction caused by antiviral ribonucleoside) score that can be readily obtained during preclinical studies that quantifies the mitochondrial toxicity potential of compounds. We suggest the possibility that patients exhibiting adverse effects during clinical trials may be more susceptible to damage by nucleoside analogs because of defects in mitochondrial or nuclear transcription. The paradigm reported here should facilitate development of ribonucleosides with a lower potential for toxicity.
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spelling pubmed-34995762012-11-19 Sensitivity of Mitochondrial Transcription and Resistance of RNA Polymerase II Dependent Nuclear Transcription to Antiviral Ribonucleosides Arnold, Jamie J. Sharma, Suresh D. Feng, Joy Y. Ray, Adrian S. Smidansky, Eric D. Kireeva, Maria L. Cho, Aesop Perry, Jason Vela, Jennifer E. Park, Yeojin Xu, Yili Tian, Yang Babusis, Darius Barauskus, Ona Peterson, Blake R. Gnatt, Averell Kashlev, Mikhail Zhong, Weidong Cameron, Craig E. PLoS Pathog Research Article Ribonucleoside analogues have potential utility as anti-viral, -parasitic, -bacterial and -cancer agents. However, their clinical applications have been limited by off target effects. Development of antiviral ribonucleosides for treatment of hepatitis C virus (HCV) infection has been hampered by appearance of toxicity during clinical trials that evaded detection during preclinical studies. It is well established that the human mitochondrial DNA polymerase is an off target for deoxyribonucleoside reverse transcriptase inhibitors. Here we test the hypothesis that triphosphorylated metabolites of therapeutic ribonucleoside analogues are substrates for cellular RNA polymerases. We have used ribonucleoside analogues with activity against HCV as model compounds for therapeutic ribonucleosides. We have included ribonucleoside analogues containing 2′-C-methyl, 4′-methyl and 4′-azido substituents that are non-obligate chain terminators of the HCV RNA polymerase. We show that all of the anti-HCV ribonucleoside analogues are substrates for human mitochondrial RNA polymerase (POLRMT) and eukaryotic core RNA polymerase II (Pol II) in vitro. Unexpectedly, analogues containing 2′-C-methyl, 4′-methyl and 4′-azido substituents were inhibitors of POLRMT and Pol II. Importantly, the proofreading activity of TFIIS was capable of excising these analogues from Pol II transcripts. Evaluation of transcription in cells confirmed sensitivity of POLRMT to antiviral ribonucleosides, while Pol II remained predominantly refractory. We introduce a parameter termed the mitovir (mitochondrial dysfunction caused by antiviral ribonucleoside) score that can be readily obtained during preclinical studies that quantifies the mitochondrial toxicity potential of compounds. We suggest the possibility that patients exhibiting adverse effects during clinical trials may be more susceptible to damage by nucleoside analogs because of defects in mitochondrial or nuclear transcription. The paradigm reported here should facilitate development of ribonucleosides with a lower potential for toxicity. Public Library of Science 2012-11-15 /pmc/articles/PMC3499576/ /pubmed/23166498 http://dx.doi.org/10.1371/journal.ppat.1003030 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open-access article distributed under the terms of the Creative Commons Public Domain declaration, which stipulates that, once placed in the public domain, this work may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose.
spellingShingle Research Article
Arnold, Jamie J.
Sharma, Suresh D.
Feng, Joy Y.
Ray, Adrian S.
Smidansky, Eric D.
Kireeva, Maria L.
Cho, Aesop
Perry, Jason
Vela, Jennifer E.
Park, Yeojin
Xu, Yili
Tian, Yang
Babusis, Darius
Barauskus, Ona
Peterson, Blake R.
Gnatt, Averell
Kashlev, Mikhail
Zhong, Weidong
Cameron, Craig E.
Sensitivity of Mitochondrial Transcription and Resistance of RNA Polymerase II Dependent Nuclear Transcription to Antiviral Ribonucleosides
title Sensitivity of Mitochondrial Transcription and Resistance of RNA Polymerase II Dependent Nuclear Transcription to Antiviral Ribonucleosides
title_full Sensitivity of Mitochondrial Transcription and Resistance of RNA Polymerase II Dependent Nuclear Transcription to Antiviral Ribonucleosides
title_fullStr Sensitivity of Mitochondrial Transcription and Resistance of RNA Polymerase II Dependent Nuclear Transcription to Antiviral Ribonucleosides
title_full_unstemmed Sensitivity of Mitochondrial Transcription and Resistance of RNA Polymerase II Dependent Nuclear Transcription to Antiviral Ribonucleosides
title_short Sensitivity of Mitochondrial Transcription and Resistance of RNA Polymerase II Dependent Nuclear Transcription to Antiviral Ribonucleosides
title_sort sensitivity of mitochondrial transcription and resistance of rna polymerase ii dependent nuclear transcription to antiviral ribonucleosides
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3499576/
https://www.ncbi.nlm.nih.gov/pubmed/23166498
http://dx.doi.org/10.1371/journal.ppat.1003030
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