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Upregulation of IL-32 Isoforms in Virologically Suppressed HIV-Infected Individuals: Potential Role in Persistent Inflammation and Transcription From Stable HIV-1 Reservoirs.


ABSTRACT: BACKGROUND:Human IL-32 is a polyfunctional cytokine that was initially reported to inhibit HIV-1 infection. However, recent data suggest that IL-32 may enhance HIV-1 replication by activating the HIV-1 primary targets, CD4 T-cells. Indeed, IL-32 is expressed in multiple isoforms, some of which are proinflammatory, whereas others are anti-inflammatory. SETTING AND METHODS:Here, we aimed to determine the relative expression of IL-32 isoforms and to test their inflammatory nature and potential to induce HIV-1 production in latently infected cells from virologically suppressed HIV-infected individuals. IL-32 and other cytokines were quantified from plasma and supernatant of CD4 T-cells by ELISA. Transcripts of IL-32 isoforms were quantified by qRT-PCR in peripheral blood mononuclear cells. The impact of recombinant human IL-32 isoforms on HIV-1 transcription was assessed in CD4 T-cells from HIV-1cART individuals by qRT-PCR. RESULTS:All IL-32 isoforms were significantly upregulated in HIV-1cART compared to HIV individuals with IL-32? representing the dominantly expressed isoform, mainly in T-cells and NK-cells. At the functional level, although IL-32? induced typical proinflammatory cytokines (IL-6 and IFN-?) in TCR-activated CD4 T-cells, IL-32? showed an anti-inflammatory profile by inducing IL-10 but not IL-6 or IFN-?. However, IL-32? showed a dual phenotype by inducing both pro- and anti-inflammatory cytokines. Interestingly, consistent with its highly pro-inflammatory nature, IL-32?, but not IL-32? or IL-32?, induced HIV-1 production in latently infected CD4 T-cells isolated from combined antiretroviral therapy-treated individuals. CONCLUSIONS:Our data report on the differential expression of IL-32 isoforms and highlight the potential role of IL-32, particularly the ? isoform, in fueling persistent inflammation and transcription of viral reservoir in HIV-1 infection.

SUBMITTER: Zaidan SM 

PROVIDER: S-EPMC6857723 | biostudies-literature | 2019 Dec

REPOSITORIES: biostudies-literature

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<h4>Background</h4>Human IL-32 is a polyfunctional cytokine that was initially reported to inhibit HIV-1 infection. However, recent data suggest that IL-32 may enhance HIV-1 replication by activating the HIV-1 primary targets, CD4 T-cells. Indeed, IL-32 is expressed in multiple isoforms, some of which are proinflammatory, whereas others are anti-inflammatory.<h4>Setting and methods</h4>Here, we aimed to determine the relative expression of IL-32 isoforms and to test their inflammatory nature and  ...[more]

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