Literature DB >> 22532673

Mutations conferring resistance to viral DNA polymerase inhibitors in camelpox virus give different drug-susceptibility profiles in vaccinia virus.

Sophie Duraffour1, Graciela Andrei, Dimitri Topalis, Marcela Krečmerová, Jean-Marc Crance, Daniel Garin, Robert Snoeck.   

Abstract

Cidofovir or (S)-HPMPC is one of the three antiviral drugs that might be used for the treatment of orthopoxvirus infections. (S)-HPMPC and its 2,6-diaminopurine counterpart, (S)-HPMPDAP, have been described to select, in vitro, for drug resistance mutations in the viral DNA polymerase (E9L) gene of vaccinia virus (VACV). Here, to extend our knowledge of drug resistance development among orthopoxviruses, we selected, in vitro, camelpox viruses (CMLV) resistant to (S)-HPMPDAP and identified a single amino acid change, T831I, and a double mutation, A314V+A684V, within E9L. The production of recombinant CMLV and VACV carrying these amino acid substitutions (T831I, A314V, or A314V+A684V) demonstrated clearly their involvement in conferring reduced sensitivity to viral DNA polymerase inhibitors, including (S)-HPMPDAP. Both CMLV and VACV harboring the A314V change showed comparable drug-susceptibility profiles to various antivirals and similar impairments in viral growth. In contrast, the single change T831I and the double change A314V+A684V in VACV were responsible for increased levels of drug resistance and for cross-resistance to viral DNA polymerase antivirals that were not observed with their CMLV counterparts. Each amino acid change accounted for an attenuated phenotype of VACV in vivo. Modeling of E9L suggested that the T→I change at position 831 might abolish hydrogen bonds between E9L and the DNA backbone and have a direct impact on the incorporation of the acyclic nucleoside phosphonates. Our findings demonstrate that drug-resistance development in two related orthopoxvirus species may impact drug-susceptibility profiles and viral fitness differently.

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Year:  2012        PMID: 22532673      PMCID: PMC3416337          DOI: 10.1128/JVI.00355-12

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  62 in total

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8.  Antiviral activity of phosphonylmethoxyalkyl derivatives of purine and pyrimidines.

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  11 in total

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4.  The vaccinia virus DNA polymerase structure provides insights into the mode of processivity factor binding.

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Review 6.  Antiviral peptides as promising therapeutic drugs.

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8.  The Role of Brincidofovir in Preparation for a Potential Smallpox Outbreak.

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9.  ST-246 is a key antiviral to inhibit the viral F13L phospholipase, one of the essential proteins for orthopoxvirus wrapping.

Authors:  Sophie Duraffour; María M Lorenzo; Gudrun Zöller; Dimitri Topalis; Doug Grosenbach; Dennis E Hruby; Graciela Andrei; Rafael Blasco; Hermann Meyer; Robert Snoeck
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10.  Poxviruses Bearing DNA Polymerase Mutations Show Complex Patterns of Cross-Resistance.

Authors:  Graciela Andrei; Pierre Fiten; Marcela Krečmerová; Ghislain Opdenakker; Dimitrios Topalis; Robert Snoeck
Journal:  Biomedicines       Date:  2022-03-01
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