AI Article Synopsis

  • Pembrolizumab is a medicine used to treat advanced skin cancer (melanoma) and may help boost the immune response against HIV.
  • In a study, a person with both metastatic melanoma and HIV received pembrolizumab, and doctors looked at changes in their immune cells and HIV levels over time.
  • Results showed an initial boost in HIV-fighting immune cells and some decrease in HIV levels, but lasting changes didn't happen, suggesting that both activating the immune system and other treatments may be needed to better fight HIV.

Article Abstract

Background: Pembrolizumab is an immune checkpoint inhibitor against programmed cell death protein-1 (PD-1) approved for therapy in metastatic melanoma. PD-1 expression is associated with a diminished functionality in HIV-1 specific-CD8 T cells. It is thought that PD-1 blockade could contribute to reinvigorate antiviral immunity and reduce the HIV-1 reservoir.

Methods: Upon metastatic melanoma diagnosis, an HIV-1-infected individual on stable suppressive antiretroviral regimen was treated with pembrolizumab. A PET-CT was performed before and one year after pembrolizumab initiation. We monitored changes in the immunophenotype and HIV-1 specific-CD8 T-cell responses during 36 weeks of treatment. Furthermore, we assessed changes in the viral reservoir by total HIV-1 DNA, cell-associated HIV-1 RNA, and ultrasensitive plasma viral load.

Results: Complete metabolic response was achieved after pembrolizumab treatment of metastatic melanoma. Activated CD8 T-cells expressing HLA-DR/CD38 transiently increased over the first nine weeks of treatment. Concomitantly, there was an augmented response of HIV-1 specific-CD8 T cells with TNF production and poly-functionality, transitioning from TNF to an IL-2 profile. Furthermore, a transient reduction of 24% and 32% in total HIV-1 DNA was observed at weeks 3 and 27, respectively, without changes in other markers of viral persistence.

Conclusions: These data demonstrate that pembrolizumab may enhance the HIV-1 specific-CD8 T-cell response, marginally affecting the HIV-1 reservoir. A transient increase of CD8 T-cell activation, TNF production, and poly-functionality resulted from PD-1 blockade. However, the lack of sustained changes in the viral reservoir suggests that viral reactivation is needed concomitantly with HIV-1-specific immune enhancement.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6947580PMC
http://dx.doi.org/10.3390/jcm8122089DOI Listing

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