Multilayered HIV-1 gag-specific T-cell responses contribute to slow progression in HLA-A(∗)30-B(∗)13-C(∗)06-positive patients

OBJECTIVE: The HLA-A(∗)30-B(∗)13-C(∗)06 haplotype is reported to be associated with slow disease progression in the HIV-1-infected Northern Han Chinese population, but the mechanism remains unknown. DESIGN: Gag-specific T-cell responses and gag sequencing were performed in nine B′ clade HIV-1-infect...

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Detalles Bibliográficos
Autores principales: Zhang, Hui, Han, Xiaoxu, Zhao, Bin, An, Minghui, Wang, Zhe, Jiang, Fanming, Xu, Junjie, Zhang, Zining, Dong, Tao, Shang, Hong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Lippincott Williams & Wilkins 2015
Materias:
Basic Science
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4444423/
https://www.ncbi.nlm.nih.gov/pubmed/25756195
http://dx.doi.org/10.1097/QAD.0000000000000652
Descripción
Sumario:OBJECTIVE: The HLA-A(∗)30-B(∗)13-C(∗)06 haplotype is reported to be associated with slow disease progression in the HIV-1-infected Northern Han Chinese population, but the mechanism remains unknown. DESIGN: Gag-specific T-cell responses and gag sequencing were performed in nine B′ clade HIV-1-infected HLA-A(∗)30-B(∗)13-C(∗)06-positive slow progressors to understand HLA-associated viral control. METHODS: Interferon-γ ELISPOT assays were performed to determine the Gag-specific T-cell responses and cross-reactivity to variant peptides. Longitudinal HIV-1 gag sequencing was performed at the clonal level. RESULTS: The overlapping peptides (OLP)-48: RQANFLGKIWPSHKGRPGNF (RL42 Gag(434-453)); OLP-2: GQLDRWEKIRLRPGGKKKYR (RL42 Gag(11-30)); OLP-15: VQNLQGQMVHQPISPRTLNA (RL42 Gag(135-154)) and OLP-16: HQPISPRTLNAWVKVVEEKA (RL42 Gag(144-163)) were dominant in HLA-A(∗)30-B(∗)13-C(∗)06-positive patients. A new epitope [HQPISPRTL (Gag(144-152), HL9)] within OLP-15 and OLP-16 was identified. Results showed that strong cross-reactive responses to multiple immunodominant peptides were associated with better clinical outcomes. In addition, efficient cross-recognition of HL9 autologous variants developed in patients was associated with high CD4(+) T-cell counts. However, two patients who had developed mutations to their dominant responses during the follow-up experienced decrease in CD4(+) T-cell counts. It appears that Gag-specific T-cell responses against one or more unmutated epitopes or cross-recognition of autologous epitope variants contribute to slow disease progression in HLA-A(∗)30-B(∗)13-C(∗)06-positive patients. CONCLUSION: We conclude that a single ‘appropriate’ Gag-specific T-cell response appears to be sufficient to protect patients from disease progression. HLA-A(∗)30-B(∗)13-C(∗)06-positive individuals benefited from having a choice of numerous immunodominant gag epitopes for T cells to react. The study offers new insight for future design of T-cell-based HIV-1 vaccine.

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