Ribavirin Reveals a Lethal Threshold of Allowable Mutation Frequency for Hantaan Virus

doi:10.1128/JVI.00874-07

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Journal of Virology, November 2007, p. 11722-11729, Vol. 81, No. 21
0022-538X/07/$08.00+0 doi:10.1128/JVI.00874-07
Copyright © 2007, American Society for Microbiology. All Rights Reserved.

Ribavirin Reveals a Lethal Threshold of Allowable Mutation Frequency for Hantaan Virus

Dong-Hoon Chung,¹ Yanjie Sun,¹ William B. Parker,¹ Jeffrey B. Arterburn,² Al Bartolucci,³ and Colleen B. Jonsson¹^*

Department of Biochemistry and Molecular Biology, 2000 9th Ave. South, Southern Research Institute, Birmingham, Alabama 35205,¹ Department of Chemistry and Biochemistry, New Mexico State University, Las Cruces, New Mexico 88003,² Department of Biostatistics, University of Alabama at Birmingham, Birmingham, Alabama 35294³

Received 24 April 2007/ Accepted 6 August 2007

The broad spectrum of antiviral activity of ribavirin (RBV)lies in its ability to inhibit IMP dehydrogenase, which lowerscellular GTP. However, RBV can act as a potent mutagen for someRNA viruses. Previously we have shown a lack of correlationbetween antiviral activity and GTP repression for Hantaan virus(HTNV) and evidence for RBV's ability to promote error-pronereplication. To further explore the mechanism of RBV, GTP levels,specific infectivity, and/or mutation frequency was measuredin the presence of RBV, mycophenolic acid (MPA), selenazofurin,or tiazofurin. While all four drugs resulted in a decrease inthe GTP levels and infectious virus, only RBV increased themutation frequency of viral RNA (vRNA). MPA, however, couldenhance RBV's mutagenic effect, which suggests distinct mechanismsof action for each. Therefore, a simple drop in GTP levels doesnot drive the observed error-prone replication. To further exploreRBV's mechanism of action, we made a comprehensive analysisof the mutation frequency over several RBV concentrations. Ofimportance, we observed that the viral population reached athreshold after which mutation frequency did not correlate witha dose-dependent decrease in the level of vRNA, PFU, or [RTP]/[GTP](where RTP is ribavirin-5'-triphosphate) over these same concentrationsof RBV. Modeling of the relationship of mutation frequency anddrug concentration showed an asymptotic relationship at thispoint. After this threshold, approximately 57% of the viralcDNA population was identical to the wild type. These studiesrevealed a lethal threshold, after which we did not observea complete loss of the quasispecies structure of the wild-typegenome, although we observed extinction of HTNV.

* Corresponding author. Mailing address: Department of Biochemistry and Molecular Biology, 2000 9th Ave. South, Southern Research Institute, Birmingham, AL 35205. Phone: (205) 581-2681. Fax: (205) 581-2093. E-mail: jonsson{at}sri.org

Published ahead of print on 15 August 2007.

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