Block-And-Lock Strategies to Cure HIV Infection

Vansant, Greet; Bruggemans, Anne; Janssens, Julie; Debyser, Zeger

doi:10.3390/v12010084

Cited by 129 publications

(125 citation statements)

References 144 publications

(186 reference statements)

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“…This work is part of a larger project aimed at developing a translatable, proof‐of‐concept cure strategy for HIV that utilizes highly specific CRISPR/dead Cas9 reagents to inactivate virus replication in both latently and actively infected cells using a “block and lock” approach, whereby viral transcription is “blocked,” “locking” proviruses in deep latency 1,2 . Here, we target a critical step in HIV transcription, that is, the interaction of the Tat protein with the TAR element in the nascent viral RNA.…”

Section: Discussionmentioning

confidence: 99%

“…However, cART does not affect the reservoir of latently infected cells, which is not sensitive to antivirals and not detected by the immune system, leading in most cases to virus rebound from this reservoir when therapy is interrupted. One strategy to potentially achieve a functional cure is the “block and lock” approach, which aims at locking out proviruses in a deep latency that prevents viral reactivation by inhibiting viral transcription 1,2 . thereby suppressing the residual viremia arising from reactivation of latently infected cells.…”

Section: Introductionmentioning

confidence: 99%

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Silencing integrated SIV proviral DNA with TAR‐specific CRISPR tools

Smith

Hodara

Parodi

et al. 2020

J of Medical Primatology

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Background One approach for a functional HIV cure is to prevent transcription from integrated proviral DNA. A critical step in HIV transcription is the Tat protein interaction with the TAR element viral RNA. We tested the strategy of blocking this Tat‐TAR interaction in the SIVmac model. Methods We designed five CRISPR short guiding RNAs (sgRNAs) targeting the SIVmac TAR element, along with inactive versions of Cas9 (dCas9). These sgRNA constructs were delivered as ribonucleoproteins or plasmid DNA, along with SIV DNA. The constructs were also tested in integrated viral DNA in a cell line chronically infected by SIV. Results The sgRNAs targeting the coding strand of the TAR element inhibited SIV RNA transcription in association with dCas9‐KRAB, but not with dCas9. Conclusions Induction of epigenetic modifications may be more effective in inactivating provirus than transcriptional interference and thus may be a better strategy to achieve a functional cure in vivo.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Silencing integrated SIV proviral DNA with TAR‐specific CRISPR tools

Smith

Hodara

Parodi

et al. 2020

J of Medical Primatology

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“…Contemporary research studies focus on the investigation of both HIV-1 and host factors to develop vaccines against HIV-1, which may represent the basis for the novel therapeutic approaches [4,5,33]. While developing new strategies of treatment can be beneficial for HIV-1 prevention and cure, antiretroviral treatment is still used worldwide, so the approaches leading to its optimization still can have an impact on the improvement of HIV-1 therapy strategies.…”

Section: Predicting Treatment Failure and Treatment Effectivenessmentioning

confidence: 99%

“…These two factors lead to a high mutation rate of HIV-1 [3]. Currently, the role of multiple HIV-1 proteins in HIV-1/AIDS disease pathogenesis and progression is under investigation, including the role of its structural proteins, as well as HIV-1 trans-activator of transcription (tat) protein [4,5]. These studies are essential because they might have an impact on the development of HIV-1 vaccines and novel therapeutic approaches (such as, for instance, "block-and-lock strategies").…”

Section: Introductionmentioning

confidence: 99%

“…ATV, Atazanavir; APV, Amprenavir; DRV, Darunavir; FPV, Fosamprenavir; IDV, Indinavir; LPV, Lopinavir; NFV, Nelfinavir; RTV, Ritonavir, SQV, Saquinavir; TPV, Tipranavir; 2 period of drug exposure: weeks, average (standard deviation) 3 AUC/ROC: area under the ROC curve obtained in leave-one-out cross-validation (LOO CV); AUC/ROC 20 , area under the ROC curve obtained in fivefold CV;4 HIV-1 PR inhibitors were taken in combination with other antiretroviral drug(s); 5 N/A data are not available.…”

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confidence: 99%

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A Computational Approach for the Prediction of Treatment History and the Effectiveness or Failure of Antiretroviral Therapy

Tarasova

Biziukova

Kireev

et al. 2020

IJMS

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Human Immunodeficiency Virus Type 1 (HIV-1) infection is associated with high mortality if no therapy is provided. Currently, the treatment of an HIV-1 positive patient requires that several drugs should be taken simultaneously. The resistance of the virus to an antiretroviral drug may lead to treatment failure. Our approach focuses on predicting the exposure of a particular viral variant to an antiretroviral drug or drug combination. It also aims at the prediction of drug treatment success or failure. We utilized nucleotide sequences of HIV-1 encoding protease and reverse transcriptase to perform such types of prediction. The PASS (Prediction of Activity Spectra for Substances) algorithm based on the naive Bayesian classifier was used to make a prediction. We calculated the probability of whether a sequence belonged (P1) or did not belong (P0) to the class associated with exposure of the viral sequence to the set of drugs that can be associated with resistance to the set of drugs. The accuracy calculated as the average Area Under the ROC (Receiver Operating Characteristic) Curve (AUC/ROC) for classifying exposure of the sequence to the HIV-1 protease inhibitors was 0.81 (±0.07), and for HIV-1 reverse transcriptase, it was 0.83 (±0.07). To predict cases of treatment effectiveness or failure, we used P1 and P0 values, obtained in PASS, along with the binary vector constructed based on short nucleotide descriptors and the applied random forest classifier. Average AUC/ROC prediction accuracy for the prediction of treatment effectiveness or failure for the combinations of HIV-1 protease inhibitors was 0.82 (±0.06) and of HIV-1 reverse transcriptase was 0.76 (±0.09).

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Garcinol from Garcinia indica inhibits HIV‐1 reverse transcriptase‐associated ribonuclease H

Corona

Seibt

Schaller

et al. 2021

Archiv der Pharmazie

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The bioactive components of Garcinia indica, garcinol (camboginol), and isogarcinol (cambogin), are suitable drug candidates for the treatment of various human diseases. HIV‐1‐RNase H assay was used to study the RNase H inhibition by garcinol and isogarcinol. Docking of garcinol into the active site of the enzyme was carried out to rationalize the difference in activities between the two compounds. Garcinol showed higher HIV‐1‐RNase H inhibition than the known inhibitor RDS1759 and retained full potency against the RNase H of a drug‐resistant HIV‐1 reverse transcriptase form. Isogarcinol was distinctly less active than garcinol, indicating the importance of the enolizable β‐diketone moiety of garcinol for anti‐RNase H activity. Docking calculations confirmed these findings and suggested this moiety to be involved in the chelation of metal ions of the active site. On the basis of its HIV‐1 reverse transcriptase‐associated RNase H inhibitory activity, garcinol is worth being further explored concerning its potential as a cost‐effective treatment for HIV patients.

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Block-And-Lock Strategies to Cure HIV Infection

Cited by 129 publications

References 144 publications

Silencing integrated SIV proviral DNA with TAR‐specific CRISPR tools

Silencing integrated SIV proviral DNA with TAR‐specific CRISPR tools

A Computational Approach for the Prediction of Treatment History and the Effectiveness or Failure of Antiretroviral Therapy

Garcinol from Garcinia indica inhibits HIV‐1 reverse transcriptase‐associated ribonuclease H

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