Sensitivity of arabinosyladenine-resistant mutants of herpes simplex virus to other antiviral drugs and mapping of drug hypersensitivity mutations to the DNA polymerase locus.

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J Virol. 1985 February; 53(2): 477-488

Sensitivity of arabinosyladenine-resistant mutants of herpes simplex virus to other antiviral drugs and mapping of drug hypersensitivity mutations to the DNA polymerase locus.

D M Coen, H E Fleming Jr, L K Leslie and M J Retondo

ABSTRACT

Seven herpes simplex virus mutants which have been previouslyshown to be resistant to arabinosyladenine were examined fortheir sensitivities to four types of antiviral drugs. Thesedrugs were a pyrophosphate analog, four nucleoside analogs alteredin their sugar moieties, two nucleoside analogs altered in theirbase moieties, and one altered in both. The seven mutants exhibitedfive distinct phenotypes based on their sensitivities to thedrugs relative to wild-type strain KOS. All mutants exhibitedresistance to acyclovir and arabinosylthymine, as well as marginalresistance to iododeoxyuridine, whereas all but one exhibitedresistance to phosphonoformic acid. The mutants exhibited eithersensitivity or hypersensitivity to other drugs tested--2'-nor-deoxyguanosine,5-methyl-2'-fluoroarauracil, 5-iodo-2'-fluoroarauracil, andbromovinyldeoxyuridine--some of which differed only slightlyfrom drugs to which the mutants were resistant. These resultssuggest ways to detect and treat arabinosyladenine-resistantisolates in the clinic. Antiviral hypersensitivity was a commonphenotype. Mutations conferring hypersensitivity to 2'-nor-deoxyguanosinein mutant PAAr5 and to bromovinyldeoxyridine in mutant tsD9were mapped to nonoverlapping regions of 1.1 and 0.8 kilobasepairs, respectively, within the herpes simplex virus DNA polymeraselocus. Thus, viral DNA polymerase mediates sensitivity to thesetwo drugs. However, we could not confirm reports of mutationsin the DNA polymerase locus conferring resistance to these twodrugs. All of the mutants exhibited altered sensitivity to twoor more types of drugs, suggesting that single mutations affectrecognition of the base, sugar, and triphosphate moieties ofnucleoside triphosphates by viral polymerase.

J Virol. 1985 February; 53(2): 477-488

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