Abstract
Reduced risk of HIV-1 infection correlated with antibody responses to the envelope variable 1 and 2 regions in the RV144 vaccine trial. To understand the relationship between antibody responses, V2 sequence, and structure, plasma samples (n = 16) from an early acute HIV-1 infection cohort from Thailand infected with CRF01_AE strain were analyzed for binding to V2 peptides by surface plasmon resonance. Five participants with a range of V2 binding responses at week 24 post-infection were further analyzed against a set of four overlapping V2 peptides that were designed based on envelope single-genome amplification. Antibody responses that were relatively consistent over the four segments of the V2 region or a focused response to the C-strand (residues 165-186) of the V2 region were observed. Viral escape in the V2 region resulted in significantly reduced antibody binding. Structural modeling indicated that the C-strand and the sites of viral variation were highly accessible in the open conformation of the HIV-1 Env trimer. V2 residues, 165-186 are preferentially targeted during acute infection. Residues 169-184 were also preferentially targeted by the protective immune response in the RV144 trial, thus emphasizing the importance of these residues for vaccine design.
Original language | English |
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Journal | Cells |
Volume | 8 |
Issue number | 4 |
DOIs | |
State | Published - 19 Apr 2019 |
Keywords
- AIDS Vaccines/administration & dosage
- Amino Acid Sequence/genetics
- Antibodies, Neutralizing/blood
- Cohort Studies
- HIV Antibodies/immunology
- HIV Envelope Protein gp120/genetics
- HIV Infections/immunology
- HIV Seropositivity
- HIV-1/immunology
- Humans
- Immunity, Humoral