par Covens, Kris;Kabeya, Kabamba 
;Schrooten, Yoeri;Dekeersmaeker, Nathalie;Van Wijngaerden, Eric;Vandamme, Anne-Mieke;De Wit, Stéphane ;Van Laethem, Kristel
Référence Journal of clinical virology, 44, 4, page (325-328)
Publication Publié, 2009-04
;Schrooten, Yoeri;Dekeersmaeker, Nathalie;Van Wijngaerden, Eric;Vandamme, Anne-Mieke;De Wit, Stéphane ;Van Laethem, KristelRéférence Journal of clinical virology, 44, 4, page (325-328)
Publication Publié, 2009-04
Article révisé par les pairs
| Résumé : | Background: Enfuvirtide is active against isolates from different HIV-1 subtypes. In vitro and in vivo studies reveal that resistance mutations are primarily found within the region spanning amino acid 36-45 of gp41. However, most studies include only subtype B strains, while it is known that especially the env region is very divergent among subtypes. Objectives: To analyze the gp41 HR1 genetic evolution during failure of enfuvirtide-containing salvage regimens in 19 HIV-1 patients infected with strains from different group M subtypes. Study design: The gp41 sequence was determined at baseline and upon failure in 19 patients. For a subset of 7 patients, samples were available after discontinuation of enfuvirtide. Results: Our results confirmed the conserved nature of the HR1 region. Escape mutants during chronic treatment with enfuvirtide were mainly observed within region 36-45. One novel mutation was identified, i.e. S42G in a subtype A1 strain. Conclusions: Different subtypes escape enfuvirtide selective pressure through similar mutational patterns, however a new S42G variant was observed. The in vivo selection of S42G suggests that it might play a role in enfuvirtide resistance. Therefore, it could be considered as a candidate mutation to be included within drug resistance interpretation systems. © 2009 Elsevier B.V. All rights reserved. |
