| Literature DB >> 29045830 |
Cari F Kessing1, Christopher C Nixon2, Chuan Li1, Perry Tsai2, Hiroshi Takata3, Guillaume Mousseau1, Phong T Ho2, Jenna B Honeycutt2, Mohammad Fallahi1, Lydie Trautmann3, J Victor Garcia4, Susana T Valente5.
Abstract
HIV-1 Tat activates viral transcription and limited Tat transactivation correlates with latency establishment. We postulated a "block-and-lock" functional cure approach based on properties of the Tat inhibitor didehydro-Cortistatin A (dCA). HIV-1 transcriptional inhibitors could block ongoing viremia during antiretroviral therapy (ART), locking the HIV promoter in persistent latency. We investigated this hypothesis in human CD4+ T cells isolated from aviremic individuals. Combining dCA with ART accelerates HIV-1 suppression and prevents viral rebound after treatment interruption, even during strong cellular activation. We show that dCA mediates epigenetic silencing by increasing nucleosomal occupancy at Nucleosome-1, restricting RNAPII recruitment to the HIV-1 promoter. The efficacy of dCA was studied in the bone marrow-liver-thymus (BLT) mouse model of HIV latency and persistence. Adding dCA to ART-suppressed mice systemically reduces viral mRNA in tissues. Moreover, dCA significantly delays and reduces viral rebound levels upon treatment interruption. Altogether, this work demonstrates the potential of block-and-lock cure strategies.Entities:
Keywords: HIV latency; HIV-1; HIV-1 transcription; Tat inhibitor; block-and-lock; didehydro-Cortistatin A; epigenetics; humanized mouse model; infected CD4+T cells; latent reservoir
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Year: 2017 PMID: 29045830 PMCID: PMC5653276 DOI: 10.1016/j.celrep.2017.09.080
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423