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Drug resistance-related mutations T369V/I in the connection subdomain of HIV-1 reverse transcriptase severely impair viral fitness.

Authors :
Wang, Zheng
Zhang, Junli
Li, Fan
Ji, Xiaolin
Liao, Lingjie
Ma, Liying
Xing, Hui
Feng, Yi
Li, Dan
Shao, Yiming
Source :
Virus Research. Apr2017, Vol. 233, p8-16. 9p.
Publication Year :
2017

Abstract

Fitness is a key parameter in the measurement of transmission capacity of individual drug-resistant HIV. Drug-resistance related mutations (DRMs) T369V/I and A371V in the connection subdomain (CN) of reverse transcriptase (RT) occur at higher frequencies in the individuals experiencing antiretroviral therapy failure. Here, we evaluated the effects of T369V/I and A371V on viral fitness, in the presence or in the absence of thymidine analogue resistance-associated mutations (TAMs) and assessed the effect of potential RT structure-related mechanism on change in viral fitness. Mutations T369V/I, A371V, alone or in combination with TAMs were introduced into a modified HIV-1 infectious clone AT1 by site-directed mutagenesis. Then, experiments on mutant and wild-type virus AT2 were performed separately using a growth-competition assay, and then the relative fitness was calculated. Structural analysis of RT was conducted using Pymol software. Results showed that T369V/I severely impaired the relative virus fitness, and A371V compensated for the viral fitness reduction caused by TAMs. Structural modeling of RT suggests that T369V/I substitutions disrupt powerful hydrogen bonds formed by T369 and V365 in p51 and p66. This study indicates that the secondary DRMs within CN might efficiently damage viral fitness, and provides valuable information for clinical surveillance and prevention of HIV-1 strains carrying these DRMs. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
01681702
Volume :
233
Database :
Academic Search Index
Journal :
Virus Research
Publication Type :
Academic Journal
Accession number :
122578952
Full Text :
https://doi.org/10.1016/j.virusres.2017.03.002