GS-9822, a preclinical LEDGIN candidate, displays a block-and-lock phenotype in cell culture

GS-9822, a preclinical LEDGIN candidate, displays a block-and-lock phenotype in cell culture

The ability of HIV to integrate into the host genome and establish latent reservoirs is the main hurdle preventing an HIV cure. LEDGINs are small-molecule integrase inhibitors that target the binding pocket of LEDGF/p75, a cellular cofactor that substantially contributes to HIV integration site sele...

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Veröffentlicht in:Antimicrobial agents and chemotherapy 2021-04, Vol.65 (5)
Hauptverfasser: Bruggemans, Anne, Vansant, Gerlinde, Balakrishnan, Mini, Mitchell, Michael L, Cai, Ruby, Christ, Frauke, Debyser, Zeger
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Antiviral Agents
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container_end_page
container_issue 5
container_start_page
container_title Antimicrobial agents and chemotherapy
container_volume 65
creator Bruggemans, Anne
Vansant, Gerlinde
Balakrishnan, Mini
Mitchell, Michael L
Cai, Ruby
Christ, Frauke
Debyser, Zeger
description The ability of HIV to integrate into the host genome and establish latent reservoirs is the main hurdle preventing an HIV cure. LEDGINs are small-molecule integrase inhibitors that target the binding pocket of LEDGF/p75, a cellular cofactor that substantially contributes to HIV integration site selection. They are potent antivirals that inhibit HIV integration and maturation. In addition, they retarget residual integrants away from transcription units and towards a more repressive chromatin environment. As a result, treatment with the LEDGIN CX14442 yielded residual provirus that proved more latent and more refractory to reactivation, supporting the use of LEDGINs as research tools to study HIV latency and a functional cure strategy. In this study we compared GS-9822, a potent, pre-clinical lead compound, with CX14442 with respect to antiviral potency, integration site selection, latency and reactivation. GS-9822 was more potent than CX14442 in most assays. For the first time, the combined effects on viral replication, integrase-LEDGF/p75 interaction, integration sites, epigenetic landscape, immediate latency and latency reversal was demonstrated at nanomolar concentrations achievable in the clinic. GS-9822 profiles as a preclinical candidate for future functional cure research.
doi_str_mv 10.1128/AAC.02328-20
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title GS-9822, a preclinical LEDGIN candidate, displays a block-and-lock phenotype in cell culture
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