GS-9822, a Preclinical LEDGIN Candidate, Displays a Block-and-Lock Phenotype in Cell Culture

Bruggemans, Anne; Vansant, Gerlinde; Balakrishnan, Mini; Mitchell, Michael; Cai, Ruby; Christ, Frauke; Debyser, Zeger

doi:10.1128/aac.02328-20

Cited by 21 publications

(35 citation statements)

References 84 publications

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“…After LEDGIN-mediated retargeting, the residual HIV-1 reservoir was shown to be more latent and less prone to reactivation ( 21 ). This result was corroborated recently using the LEDGIN GS-9822 ( 34 ), displaying activity in the low-nanomolar range, which increased immediate latency and reduced provirus reactivation at nanomolar concentrations in in vitro -infected T cell lines. Immediate latency refers to early silencing of HIV-1 expression, usually within 24 h prior to initiation of Tat-dependent HIV-1 transcription ( 35 , 36 ).…”

Section: Introductionsupporting

confidence: 70%

Single-Cell Imaging Shows That the Transcriptional State of the HIV-1 Provirus and Its Reactivation Potential Depend on the Integration Site

Janssens

Wit

Parveen

et al. 2022

mBio

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Section: Introductionsupporting

confidence: 70%

Single-Cell Imaging Shows That the Transcriptional State of the HIV-1 Provirus and Its Reactivation Potential Depend on the Integration Site

Janssens

Wit

Parveen

et al. 2022

mBio

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“…Specifically, proviruses were integrating into less-genedense regions with a more repressive epigenetic environment, and were shifted away from H3K36me3, which lowered HIV-1 transcription. Similar results were noted with GS-9822, also an ALLINI, in that residual provirus was both more latent and refractory to reactivation, and were integrated away from genes and gene-dense chromatin, resulting in a more repressive heterochromatin environment (33). Collectively, these studies suggest that if HIV-1-infected individuals are treated early with ART regimens that include an ALLINI, the replication-competent viral reservoir in resting CD4+ T cells will be transcriptionally impaired, thus mimicking a "locked" phenotype.…”

Section: Allosteric Integrase Inhibitors (Allinis)supporting

confidence: 74%

Toward a Functional Cure for HIV-1 Infection: The Block and Lock Therapeutic Approach

Vargas

Sluis‐Cremer²

2022

Front. Virol.

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The persistence of latent, replication-competent HIV-1 proviruses in resting CD4+ T cells, and other cellular reservoirs, represents a major barrier to a cure. This reservoir is impervious to the immune system and to antiretroviral therapy, but has the potential to produce infectious rebound virus if antiretroviral therapy is interrupted. There are multiple ongoing efforts to identify and/or develop novel therapeutic strategies to eliminate or silence this latent reservoir of HIV-1 infection. One of these strategies is termed “block and lock”. The “block” refers to a therapeutic agent’s capacity to inhibit (or “block”) transcription of HIV-1 proviruses, while the “lock” refers to its capacity to induce permanent silencing of the proviruses, typically via repressive epigenetic modifications. The “block and lock” approach elicits a functional, rather than sterilizing, cure for HIV-1 infection. This review article focuses on therapeutic approaches (i.e., small molecules, nucleic acids and recombinant proteins) that have been identified to block and, in some cases, lock HIV-1 in the latent state. We also touch on critical research that needs to be accomplished to advance this approach into humans.

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“…The δ-retroviral human T lymphotropic virus 1 transcriptional activator Tax protein can also significantly enhance HIV-1 transcription from unintegrated vDNA [ 136 , 137 ]. Research that aims to inform the roles of IN residues or IN inhibitors on HIV-1′s ability to replicate under physiologically relevant conditions might appropriately avoid Tax-expressing cell lines such as MT-4 and C8166-45 [ 40 , 138 , 139 , 140 , 141 , 142 , 143 , 144 ] moving forward.…”

Section: Phenotypic Spectra Of Hiv-1 In Mutant Virusesmentioning

confidence: 99%

“…Prototypical quinoline and pyridine compounds are shown in Figure 6 A. Recent studies have characterized several highly potent compounds based on expanded chemical scaffolds that inhibit HIV-1 replication in cell culture at effective concentration 50% (EC 50 ) values of ~0.4–2.5 nM [ 143 , 215 , 216 , 217 ].…”

Section: Allosteric In Inhibitorsmentioning

confidence: 99%

Multimodal Functionalities of HIV-1 Integrase

Engelman

Kvaratskhelia

2022

Viruses

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Integrase is the retroviral protein responsible for integrating reverse transcripts into cellular genomes. Co-packaged with viral RNA and reverse transcriptase into capsid-encased viral cores, human immunodeficiency virus 1 (HIV-1) integrase has long been implicated in reverse transcription and virion maturation. However, the underlying mechanisms of integrase in these non-catalytic-related viral replication steps have remained elusive. Recent results have shown that integrase binds genomic RNA in virions, and that mutational or pharmacological disruption of integrase-RNA binding yields eccentric virion particles with ribonucleoprotein complexes situated outside of the capsid shell. Such viruses are defective for reverse transcription due to preferential loss of integrase and viral RNA from infected target cells. Parallel research has revealed defective integrase-RNA binding and eccentric particle formation as common features of class II integrase mutant viruses, a phenotypic grouping of viruses that display defects at steps beyond integration. In light of these new findings, we propose three new subclasses of class II mutant viruses (a, b, and c), all of which are defective for integrase-RNA binding and particle morphogenesis, but differ based on distinct underlying mechanisms exhibited by the associated integrase mutant proteins. We also assess how these findings inform the role of integrase in HIV-1 particle maturation.

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GS-9822, a Preclinical LEDGIN Candidate, Displays a Block-and-Lock Phenotype in Cell Culture

Cited by 21 publications

References 84 publications

Single-Cell Imaging Shows That the Transcriptional State of the HIV-1 Provirus and Its Reactivation Potential Depend on the Integration Site

Single-Cell Imaging Shows That the Transcriptional State of the HIV-1 Provirus and Its Reactivation Potential Depend on the Integration Site

Toward a Functional Cure for HIV-1 Infection: The Block and Lock Therapeutic Approach

Multimodal Functionalities of HIV-1 Integrase

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