1. HLA-E–restricted HIV-1–specific CD8+ T cell responses in natural infection
- Author
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Bansal, Anju, Gehre, Mika N, Qin, Kai, Sterrett, Sarah, Ali, Ayub, Dang, Ying, Abraham, Sojan, Costanzo, Margaret C, Venegas, Leon A, Tang, Jianming, Manjunath, N, Brockman, Mark A, Yang, Otto O, Kan-Mitchell, June, and Goepfert, Paul A
- Subjects
Prevention ,Clinical Research ,HIV/AIDS ,Vaccine Related (AIDS) ,Infectious Diseases ,Vaccine Related ,Immunization ,Aetiology ,2.1 Biological and endogenous factors ,Infection ,Good Health and Well Being ,Amino Acid Sequence ,Antigen Presentation ,CD8-Positive T-Lymphocytes ,Cell Line ,HIV Infections ,HIV Seronegativity ,HIV-1 ,HLA-B Antigens ,Histocompatibility Antigens Class I ,Humans ,Immunodominant Epitopes ,In Vitro Techniques ,Receptors ,Antigen ,T-Cell ,alpha-beta ,gag Gene Products ,Human Immunodeficiency Virus ,Infectious disease ,T cells ,Medical and Health Sciences ,Immunology - 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.
- Published
- 2021