Skip NavigationSkip to Content
Return Return to Search Results

Phenotypic characterization of drug resistance-associated mutations in HIV-1 RT connection and RNase H domains and their correlation with thymidine analogue mutations

  1. Author:
    Lengruber, R. B.
    Delviks-Frankenberry, K. A.
    Nikolenko, G. N.
    Baumann, J.
    Santos, A. F.
    Pathak, V. K.
    Soares, M. A.

  2. Author Address

    [Lengruber, Renan B.; Santos, Andre F.; Soares, Marcelo A.] Univ Fed Rio de Janeiro, Dept Genet, Rio De Janeiro, Brazil. [Delviks-Frankenberry, Krista A.; Nikolenko, Galina N.; Baumann, Jessica; Pathak, Vinay K.] NCI, HIV Drug Resistance Program, Frederick, MD 21702 USA. [Soares, Marcelo A.] Inst Nacl Canc, Rio De Janeiro, Brazil.;Soares, MA, Ilha Fundao, CCS, Bloco A,Sala A2-120, BR-21949570 Rio De Janeiro, Brazil.;masoares@biologia.ufrj.br
    1. Year: 2011
    2. Date: Apr
  2. Journal: Journal of Antimicrobial Chemotherapy
    1. 66
    2. 4
    3. Pages: 702-708
  4. Type of Article: Article
  5. ISSN: 0305-7453
  1. Abstract:

    Objectives: HIV-1 reverse transcriptase (RT) mutations associated with antiviral drug resistance have been extensively characterized in the enzyme polymerase domain. Recent studies, however, have verified the involvement of the RT C-terminal domains (connection and RNase H) in drug resistance to RT inhibitors. In this work, we have characterized the correlation of recently described C-terminal domain mutations with thymidine analogue mutations (TAMs), as well as their phenotypic impact on susceptibility to zidovudine and nevirapine. Methods: HIV-1 RT sequences from Brazilian patients and from public sequence databases for which the C-terminal RT domains and treatment status were also available were retrieved and analysed for the association of C-terminal mutations and the presence of TAMs and treatment status. Several C-terminal RT mutations previously characterized were introduced by site-directed mutagenesis into an HIV-1 subtype B molecular clone in a wild-type, TAM-1 or TAM-2 pathway context. Mutants were tested for drug susceptibility to the prototypic drugs zidovudine and nevirapine. Results: Subtype B-infected patient database analysis showed that mutations N348I, A360V/T, T377M and D488E were found to be selected independently of TAMs, whereas mutations R358K, G359S, A371V, A400T, K451R and K512R increased in frequency with the number of TAMs in a dose-dependent fashion. Phenotypic analysis of C-terminal mutations showed that N348I, T369V and A371V conferred reduced susceptibility to zidovudine in the context of the TAM-1 and/or TAM-2 pathway, and also conferred dual resistance to nevirapine. Other mutations, such as D488E and Q547K, showed TAM-specific enhancement of resistance to zidovudine. Finally, mutation G359S displayed a zidovudine hypersusceptibility phenotype, both per se and when combined with A371V. Conclusions: This study demonstrates that distinct RT C-terminal mutations can act as primary or secondary drug resistance mutations, and are associated in a complex array of phenotypes with RT polymerase domain mutations.

    See More

  1. Keywords:

External Sources

  1. View Full Text
  2. DOI: 10.1093/jac/dkr005
  3. View record in Web of ScienceĀ®
  4. WOS: 000288551300003

Library Notes

  1. Fiscal Year: FY2010-2011
NCI at Frederick

You are leaving a government website.

This external link provides additional information that is consistent with the intended purpose of this site. The government cannot attest to the accuracy of a non-federal site.

Linking to a non-federal site does not constitute an endorsement by this institution or any of its employees of the sponsors or the information and products presented on the site. You will be subject to the destination site's privacy policy when you follow the link.

ContinueCancel