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  4. Counteraction of HLA-C-mediated immune control of HIV-1 by Nef
 
research article

Counteraction of HLA-C-mediated immune control of HIV-1 by Nef

Specht, Anke
•
Telenti, Amalio
•
Martinez, Raquel
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2010
Journal of Virology

A host genetic variant (-35C/T) correlates with increased human leukocyte antigen C (HLA-C) expression and improved control of HIV-1. HLA-C-mediated immunity may be particularly protective because HIV-1 is unable to remove HLA-C from the cell surface, whereas it can avoid HLA-A- and HLA-B-mediated immunity by Nef-mediated down-modulation. However, some individuals with the protective -35CC genotype exhibit high viral loads. Here, we investigated whether the ability of HIV-1 to replicate efficiently in the "protective" high-HLA-C-expression host environment correlates with specific functional properties of Nef. We found that high set point viral loads (sVLs) were not associated with the emergence of Nef variants that had acquired the ability to down-modulate HLA-C or were more effective in removing HLA-A and HLA-B from the cell surface. However, in individuals with the protective -35CC genotype we found a significant association between sVLs and the efficiency of Nef-mediated enhancement of virion infectivity and modulation of CD4, CD28, and the major histocompatibility complex class II (MHC-II)-associated invariant chain (Ii), while this was not observed in subjects with the -35TT genotype. Since the latter Nef functions all influence the stimulation of CD4(+) T helper cells by antigen-presenting cells, they may cooperate to affect both the activation status of infected T cells and the generation of an antiviral cytotoxic T-lymphocyte (CTL) response. In comparison, different levels of viremia in individuals with the common -35TT genotype were not associated with differences in Nef function but with differences in HLA-C mRNA expression levels. Thus, while high HLA-C expression may generally facilitate control of HIV-1, Nef may counteract HLA-C-mediated immune control in some individuals indirectly, by manipulating T-cell function and MHC-II antigen presentation.

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Type
research article
DOI
10.1128/JVI.00619-10
Author(s)
Specht, Anke
Telenti, Amalio
Martinez, Raquel
Fellay, Jacques  
Bailes, Elizabeth
Evans, David T.
Carrington, Mary
Hahn, Beatrice H.
Goldstein, David B.
Kirchhoff, Frank
Date Issued

2010

Publisher

American Society for Microbiology

Published in
Journal of Virology
Volume

84

Issue

14

Start page

7300

End page

11

Editorial or Peer reviewed

REVIEWED

Written at

OTHER

EPFL units
UPFELLAY  
Available on Infoscience
April 11, 2011
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/66262
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