Filgotinib suppresses HIV-1–driven gene transcription by inhibiting HIV-1 splicing and T cell activation
Yang-Hui Jimmy Yeh, … , Steven G. Deeks, Ya-Chi Ho
Yang-Hui Jimmy Yeh, … , Steven G. Deeks, Ya-Chi Ho
Published June 23, 2020
Citation Information: J Clin Invest. 2020;130(9):4969-4984. https://doi.org/10.1172/JCI137371.
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Filgotinib suppresses HIV-1–driven gene transcription by inhibiting HIV-1 splicing and T cell activation

Abstract

Despite effective antiretroviral therapy, HIV-1–infected cells continue to produce viral antigens and induce chronic immune exhaustion. We propose to identify HIV-1–suppressing agents that can inhibit HIV-1 reactivation and reduce HIV-1–induced immune activation. Using a newly developed dual-reporter system and a high-throughput drug screen, we identified FDA-approved drugs that can suppress HIV-1 reactivation in both cell line models and CD4+ T cells from virally suppressed HIV-1–infected individuals. We identified 11 cellular pathways required for HIV-1 reactivation as druggable targets. Using differential expression analysis, gene set enrichment analysis, and exon-intron landscape analysis, we examined the impact of drug treatment on the cellular environment at a genome-wide level. We identified what we believe to be a new function of a JAK inhibitor, filgotinib, that suppresses HIV-1 splicing. First, filgotinib preferentially suppresses spliced HIV-1 RNA transcription. Second, filgotinib suppresses HIV-1–driven aberrant cancer-related gene expression at the integration site. Third, we found that filgotinib suppresses HIV-1 transcription by inhibiting T cell activation and by modulating RNA splicing. Finally, we found that filgotinib treatment reduces the proliferation of HIV-1–infected cells. Overall, the combination of a drug screen and transcriptome analysis provides systematic understanding of cellular targets required for HIV-1 reactivation and drug candidates that may reduce HIV-1–related immune activation.

Authors

Yang-Hui Jimmy Yeh, Katharine M. Jenike, Rachela M. Calvi, Jennifer Chiarella, Rebecca Hoh, Steven G. Deeks, Ya-Chi Ho

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Figure 4

HIV-1–suppressing agents reduce HIV-1–driven aberrant host gene transcription at the integration site.

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HIV-1–suppressing agents reduce HIV-1–driven aberrant host gene transcri...
(A) Normalized transcriptional landscape using first exon at the HIV-1 integration site (proto-oncogene VAV1) in the HIV-1–Jurkat clone 8B10 treated with HIV-1–suppressing agents (10 μM) for 24 hours. HIV-1 integration into VAV1 has been previously reported in CD4+ T cells from virally suppressed HIV-1–infected individuals (72). Red arrowheads, HIV-1 integration site mapped by inverse PCR (58). (B) Western blot of VAV1 protein expression in HIV-1–infected Jurkat clone 8B10 treated with HIV-1–suppressing agents. (C) Relative quantification of intact VAV1 and truncated VAV1 expression to DMSO treatment normalized to GAPDH in triplicates. DM, DMSO; Fi, filgotinib; Ru, ruxolitinib; Sp, spironolactone; MA, mycophenolic acid. P value was calculated with 1-way ANOVA with Fisher’s least significant difference test for comparison between each treatment and DMSO control.