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Increased HIV-1 vaccine efficacy against viruses with genetic signatures in Env V2.

Authors :
Rolland M
Edlefsen PT
Larsen BB
Tovanabutra S
Sanders-Buell E
Hertz T
deCamp AC
Carrico C
Menis S
Magaret CA
Ahmed H
Juraska M
Chen L
Konopa P
Nariya S
Stoddard JN
Wong K
Zhao H
Deng W
Maust BS
Bose M
Howell S
Bates A
Lazzaro M
O'Sullivan A
Lei E
Bradfield A
Ibitamuno G
Assawadarachai V
O'Connell RJ
deSouza MS
Nitayaphan S
Rerks-Ngarm S
Robb ML
McLellan JS
Georgiev I
Kwong PD
Carlson JM
Michael NL
Schief WR
Gilbert PB
Mullins JI
Kim JH
Source :
Nature [Nature] 2012 Oct 18; Vol. 490 (7420), pp. 417-20. Date of Electronic Publication: 2012 Sep 10.
Publication Year :
2012

Abstract

The RV144 trial demonstrated 31% vaccine efficacy at preventing human immunodeficiency virus (HIV)-1 infection. Antibodies against the HIV-1 envelope variable loops 1 and 2 (Env V1 and V2) correlated inversely with infection risk. We proposed that vaccine-induced immune responses against V1/V2 would have a selective effect against, or sieve, HIV-1 breakthrough viruses. A total of 936 HIV-1 genome sequences from 44 vaccine and 66 placebo recipients were examined. We show that vaccine-induced immune responses were associated with two signatures in V2 at amino acid positions 169 and 181. Vaccine efficacy against viruses matching the vaccine at position 169 was 48% (confidence interval 18% to 66%; P = 0.0036), whereas vaccine efficacy against viruses mismatching the vaccine at position 181 was 78% (confidence interval 35% to 93%; P = 0.0028). Residue 169 is in a cationic glycosylated region recognized by broadly neutralizing and RV144-derived antibodies. The predicted distance between the two signature sites (21 ± 7 Å) and their match/mismatch dichotomy indicate that multiple factors may be involved in the protection observed in RV144. Genetic signatures of RV144 vaccination in V2 complement the finding of an association between high V1/V2-binding antibodies and reduced risk of HIV-1 acquisition, and provide evidence that vaccine-induced V2 responses plausibly had a role in the partial protection conferred by the RV144 regimen.

Details

Language :
English
ISSN :
1476-4687
Volume :
490
Issue :
7420
Database :
MEDLINE
Journal :
Nature
Publication Type :
Academic Journal
Accession number :
22960785
Full Text :
https://doi.org/10.1038/nature11519