2002
DOI: 10.1021/bi0121858
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Insights into the Molecular Mechanism of Inhibition and Drug Resistance for HIV-1 RT with Carbovir Triphosphate

Abstract: Abacavir (1592U89, or Ziagen) is a powerful and selective inhibitor of HIV-1 viral replication that has been approved by the FDA for treatment of acquired immunodeficiency syndrome. Abacavir is metabolized to the active compound carbovir triphosphate (CBVTP). This compound is a guanosine analogue containing a 2',3'-unsaturation in its planar carbocyclic deoxyribose ring that acts on HIV-1 reverse transcriptase (RT(WT)) as a molecular target, resulting in chain termination of DNA synthesis. A single amino acid … Show more

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Cited by 42 publications
(46 citation statements)
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“…Such aphidicolin-resistant viruses exhibit altered sensitivities to other substrate analogues (17). Sequence analysis and marker transfer experiments located point mutations within the conserved regions of both HSV and vaccinia virus DNApols, which conferred resistance to aphidicolin (10,22,47 (4,16,35,36,38,45).The aim of this study was to select and characterize AcMNPV mutants resistant to antiviral compounds that target the viral DNApol enzyme. We hypothesized that "escape" mutants selected from the serial passage of the parental AcMNPV in the presence of increasing concentrations of these drugs would harbor mutation(s) in the AcMNPV genome, particularly within the DNA polymerase gene (dnapol).…”
mentioning
confidence: 99%
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“…Such aphidicolin-resistant viruses exhibit altered sensitivities to other substrate analogues (17). Sequence analysis and marker transfer experiments located point mutations within the conserved regions of both HSV and vaccinia virus DNApols, which conferred resistance to aphidicolin (10,22,47 (4,16,35,36,38,45).The aim of this study was to select and characterize AcMNPV mutants resistant to antiviral compounds that target the viral DNApol enzyme. We hypothesized that "escape" mutants selected from the serial passage of the parental AcMNPV in the presence of increasing concentrations of these drugs would harbor mutation(s) in the AcMNPV genome, particularly within the DNA polymerase gene (dnapol).…”
mentioning
confidence: 99%
“…Such aphidicolin-resistant viruses exhibit altered sensitivities to other substrate analogues (17). Sequence analysis and marker transfer experiments located point mutations within the conserved regions of both HSV and vaccinia virus DNApols, which conferred resistance to aphidicolin (10,22,47 (4,16,35,36,38,45).…”
mentioning
confidence: 99%
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“…Its efficiency of incorporation is six-and 9.6-fold less than dCTP during DNA-and RNA-directed incorporation, respectively (Table 1). This is in contrast to D-D4TTP and D-D4GTP which are effective at mimicking their corresponding natural nucleotides (Vaccaro et al, 1999;Ray et al, 2002b). These results suggest that there may be base specific interactions important in nucleotide analogue incorporation.…”
Section: Kinetic Consequences Of 5-and 2′-fluorine Addition On Hiv-1mentioning
confidence: 75%
“…In general, a number of studies with HIV-1 RT have noted that the efficiency is higher for RNA-directed versus DNA-directed incorporation although the molecular mechanism has remained elusive (Kerr & Anderson, 1997;Vaccaro et al, 1999;Ray et al, 2002b). An unpublished crystal structure of RT bound to TTP and a DNA/RNA primer/template offers no further clues, as the distances between many important amino acids and TTP remain unchanged (SC Harrison, Harvard University, Mass., USA, personal communication).…”
Section: Structural Implications For the Kinetic Datamentioning
confidence: 99%