Maintenance of the HIV Reservoir Is Antagonized by Selective BCL2 Inhibition

Cummins, Nathan W.; Sainski-Nguyen, Amy; Natesampillai, Sekar; Aboulnasr, Fatma; Kaufmann, Scott H.; Badley, Andrew D.

doi:10.1128/jvi.00012-17

Cited by 60 publications

(53 citation statements)

References 67 publications

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“…Whether combinations of Bcl-2 inhibitors like Venetoclax with LRAs that do not induce maximal T-cell stimulation also lead to the death of latently infected cells remains unclear. Interestingly, Venetoclax also leads to the selective killing of HIV infected primary T-cells during productive infection in vitro (Cummins et al, 2017) and therefore Venetoclax could also potentially be used to reduce the establishment of latency.…”

Section: Pro-apoptotic Compounds To Clear Hiv Latently Infected T-cellsmentioning

confidence: 99%

“…Fourth, the effect of these compounds on dividing and non-dividing cells should be evaluated to determine how effectively various HIV infected cell types will be cleared. To this end, a recent study found that the Bcl-2 inhibitor Venetoclax induced apoptosis of the latently infected J-Lat10.6 T cell line model (Cummins et al, 2017), in which the J-Lat10.6 cells proliferate slowly in the absence of stimulation. While Venetoclax can induce apoptosis in both dividing and non-dividing HIV infected T cells, it will be important to evaluate the impact of any kill compounds on diverse cell types to ascertain selective clearance of HIV infected cells.…”

Section: Potential Challengesmentioning

confidence: 99%

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Getting the “Kill” into “Shock and Kill”: Strategies to Eliminate Latent HIV

Kim

Anderson

Lewin

2018

Cell Host & Microbe

312

351

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Despite the success of antiretroviral therapy (ART), there is currently no HIV cure and treatment is lifelong. HIV persists during ART due to long lived and proliferating latently infected CD4+ T-cells. One strategy to eliminate latency is to activate virus production using latency reversing agents (LRAs) with the goal of triggering cell death through virus-induced cytolysis or immune-mediated clearance. However, multiple studies have demonstrated that activation of viral transcription alone is insufficient to induce cell death and some LRAs may counteract cell death by promoting cell survival. Here, we review new approaches to induce death of latently infected cells through apoptosis and inhibition of pathways critical for cell survival, which are often hijacked by HIV proteins. Given advances in the commercial development of compounds that induce apoptosis in cancer chemotherapy, these agents could move rapidly into clinical trials, either alone or in combination with LRAs, to eliminate latent HIV infection.

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Section: Pro-apoptotic Compounds To Clear Hiv Latently Infected T-cellsmentioning

confidence: 99%

Section: Potential Challengesmentioning

confidence: 99%

Getting the “Kill” into “Shock and Kill”: Strategies to Eliminate Latent HIV

Kim

Anderson

Lewin

2018

Cell Host & Microbe

312

351

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“…Recently, cellular survival programs governed by BIRC5, a molecular inhibitor of apoptosis, were shown to support long-term survival of HIVinfected CD4+ T cells (63). Moreover, the Bcl-2 family has long been implicated in balancing lowlevel HIV virus production with cell survival (64)(65)(66)(67). We further showed that reactivating infected (p24+) cells express higher levels of anti-apoptotic p-Bad than latently infected (p24-) cells, suggesting that activation of viral protein expression may complicate eradication efforts.…”

Section: Discussionmentioning

confidence: 99%

Systems analysis by mass cytometry identifies susceptibility of latent HIV-infected T cells to targeting of p38 and mTOR pathways

Spudich

et al. 2018

Preprint

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Efforts to cure HIV are hindered by viral persistence in latently infected memory CD4+ T cells.Targeting T cell death pathways dysregulated by HIV infection offers a novel approach for eradication of the latent reservoir. To identify potential therapeutic targets, we compared signaling and apoptosis in uninfected and latently infected primary cultured CD4+ central memory T cells by mass cytometry following T cell receptor stimulation. We found that HIV-infected cells were sensitized to activation of pro-apoptotic p38 kinase signaling via p53, and to inhibition of antiapoptotic mTOR kinase signaling, even without HIV protein expression. Simultaneous targeting of p38 and mTOR kinases in resting CD4+ T cells from virally-suppressed HIV+ patients ex vivo reduced cell-associated HIV RNA and DNA. Our results demonstrate how systems biology approaches are useful for identifying novel therapeutic approaches to treat HIV latency, and further suggest that it may be possible to deplete latent HIV-infected T cells without viral reactivation.

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“…Similarly, targeting BCL-2 with the BH3-mimetic compound ABT-199 induces apoptosis of T-cells harboring latent but also productive HIV infections. 133 This reduces the HIV reservoir and the spreading of infections in ex vivo models. Inducing apoptosis also decreases hepatitis B viral loads in preclinical infection models.…”

Section: Targeting Apoptotic Factors To Treat Infectionsmentioning

confidence: 99%

Targeting apoptosis pathways in infections

Naderer

Fulcher

2018

Journal of Leukocyte Biology

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The programmed cell death pathway of apoptosis is essential for mammalian development and immunity as it eliminates unwanted and dangerous cells. As part of the cellular immune response, apoptosis removes the replicative niche of intracellular pathogens and enables the resolution of infections. To subvert apoptosis, pathogens have evolved a diverse range of mechanisms. In some circumstances, however, pathogens express effector molecules that induce apoptotic cell death. In this review, we focus on selected host-pathogen interactions that affect apoptotic pathways. We discuss how pathogens control the fate of host cells and how this determines the outcome of infections. Finally, small molecule inhibitors that activate apoptosis in cancer cells can also induce apoptotic cell death of infected cells. This suggests that targeting host death factors to kill infected cells is a potential therapeutic option to treat infectious diseases.

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Maintenance of the HIV Reservoir Is Antagonized by Selective BCL2 Inhibition

Cited by 60 publications

References 67 publications

Getting the “Kill” into “Shock and Kill”: Strategies to Eliminate Latent HIV

Getting the “Kill” into “Shock and Kill”: Strategies to Eliminate Latent HIV

Systems analysis by mass cytometry identifies susceptibility of latent HIV-infected T cells to targeting of p38 and mTOR pathways

Targeting apoptosis pathways in infections

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