HIV-1 Tat and Viral Latency: What We Can Learn from Naturally Occurring Sequence Variations

Kamori, Doreen; Ueno, Takamasa

doi:10.3389/fmicb.2017.00080

Cited by 38 publications

(41 citation statements)

References 85 publications

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“…Since HIV-1 Tat protein plays a key role in viral transcriptional elongation through the interaction with positive transcription elongation factor b (P-TEFb) complex, composed of cyclin T1 and cyclin-dependent kinase 9 (Kamori and Ueno, 2017), we first determined the effect of levosimendan on Tat protein level and Tat-P-TEFb protein interaction in Tat-expressing HeLa cells. Neither the Tat protein level nor the Tat-P-TEFb protein interaction was affected by the treatment of levosimedan (Figure 5A–B).…”

Section: Resultsmentioning

confidence: 99%

Screening of an FDA-approved compound library identifies levosimendan as a novel anti-HIV-1 agent that inhibits viral transcription

et al. 2017

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Combination antiretroviral therapy (cART) has been proven to efficiently inhibit ongoing replication of human immunodeficiency virus type 1 (HIV-1), and significantly improve the health outcome in patients of acquired immune deficiency syndrome (AIDS). However, cART is unable to cure HIV-1/AIDS. Even in presence of cART there exists a residual viremia, contributed from the viral reservoirs of latently infected HIV-1 proviruses; this constitutes a major hurdle. Currently, there are multiple strategies aimed at eliminating or permanently silence these HIV-1 latent reservoirs being intensely explored. One such strategy, a recently emerged “block and lock” approach is appealing. For this approach, so-called HIV-1 latency-promoting agents (LPAs) are used to reinforce viral latency and to prevent the low-level or sporadic transcription of integrated HIV-1 proviruses. Although several LPAs have been reported, there is still a question of their suitability to be further developed as a safe and valid therapeutic agent for the clinical use. In this study, we aimed to identify new potential LPAs through the screening an FDA-approved compound library. A new and promising anti-HIV-1 inhibitor, levosimendan, was identified from these screens. Levosimendan is currently used to treat heart failure in clinics, but it demonstrates strong inhibition of TNFα-induced HIV-1 reactivation in multiple cell lines of HIV-1 latency through affecting the HIV-1 Tat-LTR transcriptional axis. Furthermore, we confirmed that in primary CD4+ T cells levosimendan inhibits both the acute HIV-1 replication and the reactivation of latent HIV-1 proviruses. As a summary, our studies successfully identify levosimendan as a novel and promising anti-HIV-1 inhibitor, which should be immediately investigated in vivo given that it is already an FDA-approved drug.

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Section: Resultsmentioning

confidence: 99%

Screening of an FDA-approved compound library identifies levosimendan as a novel anti-HIV-1 agent that inhibits viral transcription

et al. 2017

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“…159,160 P-TEFb is a protein complex containing cyclin T1 and CDK9 kinase, which phosphorylates the carboxylterminal domain of the RNA Pol II recruited at the 5¢ LTR, enhancing in turn its transcription elongation activity. 159,161 However, most P-TEFb molecules are held catalytically inactive through their association with the 7SK small nuclear ribonucleoprotein (snRNP) complex. Tat promotes P-TEFb dissociation from 7SK, allowing P-TEFb to become catalytically active, hyperphosphorylate RNA Pol II, and release the transcriptional pause.…”

Section: Tat and Rna Elongationmentioning

confidence: 99%

“…From this point on, and due to a positive feedback, a highly efficient Tat-dependent HIV-1 transcription phase begins by the mechanisms described above. 82,159,161,162,172 Additionally, Tat recruits chromatinremodeling factors, such as SWI/SNF, which facilitate transcription by promoting DNA relaxation and consequently nuc-1 remodeling. 173 Tat's role in latency has been extensively documented.…”

Section: Tat and Rna Elongationmentioning

confidence: 99%

“…173 Tat's role in latency has been extensively documented. 159,174 For instance, Tat protein alone was found to be sufficient to successfully reactivate HIV-1 transcription in latently infected CD4 + T cells isolated from patients undergoing cART. 159,175,176 This was demonstrated by delivering tat either by transduction with non-HIV vectors, 176 or by ectopically delivering recombinant Tat protein to these cells.…”

Section: Tat and Rna Elongationmentioning

confidence: 99%

“…159,174 For instance, Tat protein alone was found to be sufficient to successfully reactivate HIV-1 transcription in latently infected CD4 + T cells isolated from patients undergoing cART. 159,175,176 This was demonstrated by delivering tat either by transduction with non-HIV vectors, 176 or by ectopically delivering recombinant Tat protein to these cells. 175 In this particular case, a soluble Tat-GFP chimeric protein was produced from pancreatic cells of transgenic mice, and delivered to primary, latently infected CD4 + T cells of patients undergoing cART.…”

Section: Tat and Rna Elongationmentioning

confidence: 99%

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Thirty-five years after the identification of HIV-1 as the causative agent of AIDS, we are still in search of vaccines and treatments to eradicate this devastating infectious disease. Progress has been made in understanding the molecular pathogenesis of this infection, which has been crucial for the development of the current therapy regimens. However, despite their efficacy at limiting active viral replication, these drugs are unable to purge the latent reservoir: a pool of cells that harbor transcriptionally inactive, but replication-competent HIV-1 proviruses, and that represent the main barrier to eradicate HIV-1 from affected individuals. In this review, we discuss advances in the field that have allowed a better understanding of HIV-1 latency, including the diverse cell types that constitute the latent reservoir, factors influencing latency, tools to study HIV-1 latency, as well as current and prospective therapeutic approaches to target these latently infected cells, so a functional cure for HIV/AIDS can become a reality.

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HIV-1 Tat and Viral Latency: What We Can Learn from Naturally Occurring Sequence Variations

Cited by 38 publications

References 85 publications

Screening of an FDA-approved compound library identifies levosimendan as a novel anti-HIV-1 agent that inhibits viral transcription

Screening of an FDA-approved compound library identifies levosimendan as a novel anti-HIV-1 agent that inhibits viral transcription

Barriers for HIV Cure: The Latent Reservoir

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