The differential short- and long-term effects of HIV-1 latency-reversing agents on T cell function
نویسندگان
چکیده
Despite the extraordinary success of HIV-1 antiretroviral therapy in prolonging life, infected individuals face lifelong therapy because of a reservoir of latently-infected cells that harbor replication competent virus. Recently, compounds have been identified that can reverse HIV-1 latency in vivo. These latency- reversing agents (LRAs) could make latently-infected cells vulnerable to clearance by immune cells, including cytolytic CD8+ T cells. We investigated the effects of two leading LRA classes on CD8+ T cell phenotype and function: the histone deacetylase inhibitors (HDACis) and protein kinase C modulators (PKCms). We observed that relative to HDACis, the PKCms induced much stronger T cell activation coupled with non-specific cytokine production and T cell proliferation. When examining antigen-specific CD8+ T cell function, all the LRAs except the HDACi Vorinostat reduced, but did not abolish, one or more measurements of CD8+ T cell function. Importantly, the extent and timing of these effects differed between LRAs. Panobinostat had detrimental effects within 10 hours of drug treatment, whereas the effects of the other LRAs were observed between 48 hours and 5 days. These observations suggest that scheduling of LRA and CD8+ T cell immunotherapy regimens may be critical for optimal clearance of the HIV-1 reservoir.
منابع مشابه
Corrigendum: The differential short- and long-term effects of HIV-1 latency-reversing agents on T cell function
“We thank all the study participants. For technical assistance we thank Kuo Yang and members of the UNC Clinical Trials Unit, the UNC CFAR Immunology Core and the UNC Flow Cytometry Core Facility. This study was supported by NIH grants to the Collaboratory of AIDS Researchers for Eradication (CARE; U19 AI096113) and the UNC Center for AIDS Research (CFAR; P30 AI50410). This research was also su...
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