The TLR7/IRF-5 axis sensitizes memory CD4+ T cells to Fas-mediated apoptosis during HIV-1 infection
Liseth Carmona-Pérez, Xavier Dagenais-Lussier, Linh T. Mai, Tanja Stögerer, Sharada Swaminathan, Stéphane Isnard, Matthew R. Rice, Betsy J. Barnes, Jean-Pierre Routy, Julien van Grevenynghe, Simona Stäger
Liseth Carmona-Pérez, Xavier Dagenais-Lussier, Linh T. Mai, Tanja Stögerer, Sharada Swaminathan, Stéphane Isnard, Matthew R. Rice, Betsy J. Barnes, Jean-Pierre Routy, Julien van Grevenynghe, Simona Stäger
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Research Article AIDS/HIV Immunology

The TLR7/IRF-5 axis sensitizes memory CD4+ T cells to Fas-mediated apoptosis during HIV-1 infection

Abstract

HIV-1 infection is characterized by inflammation and a progressive decline in CD4+ T cell count. Despite treatment with antiretroviral therapy (ART), the majority of people living with HIV (PLWH) maintain residual levels of inflammation, a low degree of immune activation, and higher sensitivity to cell death in their memory CD4+ T cell compartment. To date, the mechanisms responsible for this high sensitivity remain elusive. We have identified the transcription factor IRF-5 to be involved in impairing the maintenance of murine CD4+ T cells during chronic infection. Here, we investigate whether IRF-5 also contributes to memory CD4+ T cell loss during HIV-1 infection. We show that TLR7 and IRF-5 were upregulated in memory CD4+ T cells from PLWH, when compared with naturally protected elite controllers and HIVfree participants. TLR7 was upstream of IRF-5, promoting Caspase 8 expression in CD4+ T cells from ART HIV-1+ but not from HIVfree donors. Interestingly, the TLR7/IRF-5 axis acted synergistically with the Fas/FasL pathway, suggesting that TLR7 and IRF-5 expression in ART HIV-1+ memory CD4+ T cells represents an imprint that predisposes cells to Fas-mediated apoptosis. This predisposition could be blocked using IRF-5 inhibitory peptides, suggesting IRF-5 blockade as a possible therapy to prevent memory CD4+ T cell loss in PLWH.

Authors

Liseth Carmona-Pérez, Xavier Dagenais-Lussier, Linh T. Mai, Tanja Stögerer, Sharada Swaminathan, Stéphane Isnard, Matthew R. Rice, Betsy J. Barnes, Jean-Pierre Routy, Julien van Grevenynghe, Simona Stäger

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Figure 6

IRF-5 inhibitory peptides rescue memory CD4+ T cells from Fas-mediated apoptosis.

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IRF-5 inhibitory peptides rescue memory CD4+ T cells from Fas-mediated a...
(AC) Purified CD4+ T cells from ART HIV-1+ and HIVfree individuals were pretreated with 10 μM of IRF-5–CPPs for 30 minutes before stimulation with IMQ and incubated at 37°C for 30 hours. Graphs show (A) the percentage of apoptotic cells, (B) the percentage of dead cells, and (C) CASP8 mRNA expression levels in memory CD4+ T cells from ART HIV-1+ and HIVfree donors. (D) Experimental design. Purified CD4+ T cells from ART HIV-1+ and HIVfree individuals were pretreated with 10 μM of IRF-5–CPPs for 30 minutes, stimulated with or without IMQ for 12 hours, and incubated for a further 18 hours with or without rFasL. (EG) Graphs show (E) the percentage of apoptotic cells, (F) the percentage of dead cells, and (G) CASP8 mRNA expression levels in memory CD4+ T cells from ART HIV-1+ and HIVfree donors. Data are presented as the mean ± SD. The Friedman’s followed by the Dunn’s multiple-comparison tests were used for significance. *P < 0.05. n = 6.