HLA-E–restricted HIV-1–specific CD8+ T cell responses in natural infection
Anju Bansal, Mika N. Gehre, Kai Qin, Sarah Sterrett, Ayub Ali, Ying Dang, Sojan Abraham, Margaret C. Costanzo, Leon A. Venegas, Jianming Tang, N. Manjunath, Mark A. Brockman, Otto O. Yang, June Kan-Mitchell, Paul A. Goepfert
Anju Bansal, Mika N. Gehre, Kai Qin, Sarah Sterrett, Ayub Ali, Ying Dang, Sojan Abraham, Margaret C. Costanzo, Leon A. Venegas, Jianming Tang, N. Manjunath, Mark A. Brockman, Otto O. Yang, June Kan-Mitchell, Paul A. Goepfert
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Research Article Infectious disease

HLA-E–restricted HIV-1–specific CD8+ T cell responses in natural infection

Abstract

CD8+ T cell responses restricted by MHC-E, a nonclassical MHC molecule, have been associated with protection in an SIV/rhesus macaque model. The biological relevance of HLA-E–restricted CD8+ T cell responses in HIV infection, however, remains unknown. In this study, CD8+ T cells responding to HIV-1 Gag peptides presented by HLA-E were analyzed. Using in vitro assays, we observed HLA-E–restricted T cell responses to what we believe to be a newly identified subdominant Gag-KL9 as well as a well-described immunodominant Gag-KF11 epitope in T cell lines derived from chronically HIV-infected patients and also primed from healthy donors. Blocking of the HLA-E/KF11 binding by the B7 signal peptide resulted in decreased CD8+ T cell responses. KF11 presented via HLA-E in HIV-infected cells was recognized by antigen-specific CD8+ T cells. Importantly, bulk CD8+ T cells obtained from HIV-infected individuals recognized infected cells via HLA-E presentation. Ex vivo analyses at the epitope level showed a higher responder frequency of HLA-E–restricted responses to KF11 compared with KL9. Taken together, our findings of HLA-E–restricted HIV-specific immune responses offer intriguing and possibly paradigm-shifting insights into factors that contribute to the immunodominance of CD8+ T cell responses in HIV infection.

Authors

Anju Bansal, Mika N. Gehre, Kai Qin, Sarah Sterrett, Ayub Ali, Ying Dang, Sojan Abraham, Margaret C. Costanzo, Leon A. Venegas, Jianming Tang, N. Manjunath, Mark A. Brockman, Otto O. Yang, June Kan-Mitchell, Paul A. Goepfert

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Figure 2

Recognition of KF11 in the context of HLA-E*01 by non-NK/NKT CD8+ T cells from HIV-infected individuals, using the 221ΔE cell panel and in vitro–generated CD8+ T cell lines.

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Recognition of KF11 in the context of HLA-E*01 by non-NK/NKT CD8+ T cell...
(A) In vitro–cultured CD8+ T cells from 4 chronically HIV-infected individuals (CHI-12, CHI-2, CHI-4, and CHI-24) were tested for upregulation of CD107a/b in CD94-expressing CD8+ T cells in response to KF11 (10 μg/mL). APCs or target cells included 221ΔE.E*01, 221ΔE.B*57, and 221ΔE, the latter serving as a negative control. In addition, within each APC, KF11 stimulation was assessed in comparison with no-peptide-pulse control (red boxes). (B) Two different blocking strategies in patient CHI-24 were used to confirm that KF11 was presented in the context of HLA-E. KF11-specific activation of CD8+ T cells (IFN-γ production) in the context of HLA-E*01:03 but not HLA-B*57:03 was blocked by excess leader sequence B7sp peptide or by the HLA-E–specific 3D12 mAb, both at 10 μg/mL.