A mutation in helicase motif IV of herpes simplex virus type 1 UL5 that results in reduced growth in vitro and lower virulence in a murine infection model is related to the predicted helicase structure
Author:
Affiliation:
1. Department of Veterinary Medicine, University of Cambridge, Cambridge, UK
2. Department of Biochemistry, University of Cambridge, Cambridge, UK
Abstract
Publisher
Microbiology Society
Subject
Virology
Reference26 articles.
1. Single amino acid substitutions in the HSV-1 helicase protein that confer resistance to the helicase-primase inhibitor BAY 57–1293 are associated with increased or decreased virus growth characteristics in tissue culture;Biswas;Arch Virol,2007a
2. Detection of HSV-1 variants highly resistant to the helicase-primase inhibitor BAY 57-1293 at high frequency in two of ten recent clinical isolates of HSV-1;Biswas;J Antimicrob Chemother,2007b
3. Herpes simplex virus helicase-primase inhibitors: recent findings from the study of drug-resistance mutations;Biswas;Antivir Chem Chemother,2008
4. Mutations close to functional motif IV in HSV-1 UL5 helicase that confer resistance to HSV helicase-primase inhibitors, variously affect virus growth rate and pathogenicity;Biswas;Antiviral Res,2008a
5. A single drug-resistance mutation in HSV-1 UL52 primase points to a difference between two helicase-primase inhibitors in their mode of interaction with the antiviral target;Biswas;J Antimicrob Chemother,2008b
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