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Abstract

Mucosal-associated invariant T (MAIT) cell populations are reduced in frequency in HIV-1+ patients, and this disruption is associated with systemic immune activation. Reconstitution of MAIT frequency may benefit HIV-1-infected individuals; however, only recently has in vivo work been endeavored. Treatment with interleukin (IL)-2, granulocyte-macrophage colony-stimulating factor (GM-CSF), and recombinant human growth hormone (rhGH) immunotherapy combined with an HIV-1 vaccine in the context of antiretroviral therapy (ART) has shown to reconstitute CD4 T cell population numbers and function. In this study cryopreserved peripheral blood mononuclear cells (PBMCs) from 12 HIV-1+ patients who were undergoing a combination of HIV-1 vaccine and/or IL-2, GM-CSF and rhGH immunotherapy in conjunction with ART were analyzed to assess the potential of this treatment to promote MAIT cell proliferation. PBMCs were thawed from study baseline, weeks 2 and 48 time points, fluorescently stained for MAIT cell markers, and assessed by flow cytometric analysis. Matched pairs and intergroup results were statistically compared using appropriate methods. MAIT cell frequency was increased from baseline at 48 weeks in participants who received vaccine only, whereas individuals receiving IL-2, GM-CSF, and rhGH immunotherapy with or without vaccine did not show additional benefit. Although IL-2, GM-CSF, and rhGH treatment promotes CD4 T cell reconstitution and HIV-1-specific T cell function, it does not support MAIT cell recovery in patients on suppressive ART. Therapeutic immunization however has a positive effect, highlighting the importance of aiming for balanced promotion of T cell population reconstitution to impact on HIV-1 transmission and pathogenesis.

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References

Gold

, Cerri

, Smyk-Pearson

, et al.: Human mucosal associated invariant T cells detect bacterially infected cells. PLoS Biol, 2010; 8:e1000407.

Treiner

, Duban

, Bahram

, et al.: Selection of evolutionarily conserved mucosal-associated invariant T cells by MR1. Nature, 2003; 422:164–169.

Le Bourhis

, Martin

, Péguillet

, et al.: Antimicrobial activity of mucosal-associated invariant T cells. Nat Immunol, 2010; 11:701–708.

Dusseaux

, Martin

, Serriari

, et al.: Human MAIT cells are xenobiotic-resistant, tissue-targeted, CD161hi IL-17-secreting T cells. Blood, 2011; 117:1250–1259.

Greathead

, Metcalf

, Gazzard

, Gotch

, Steel

, Kelleher

: CD8+/CD161++ mucosal-associated invariant T-cell levels in the colon are restored on long-term antiretroviral therapy and correlate with CD8+ T-cell immune activation. AIDS, 2014; 28:1690–1692.

Wong

, Ndung'u

, Kasprowicz

: The role of mucosal-associated invariant T cells in infectious diseases. Immunology, 2017; 150:45–54.

Leeansyah

, Ganesh

, Quigley

, et al.: Activation, exhaustion, and persistent decline of the antimicrobial MR1-restricted MAIT-cell population in chronic HIV-1 infection. Blood, 2013; 121:1124–1135.

Leeansyah

, Svärd

, Dias

, et al.: Arming of MAIT cell cytolytic antimicrobial activity is induced by IL-7 and defective in HIV-1 infection. PLoS Pathog, 2015; 11:e1005072.

Sortino

, Richards

, Dias

, Leeansyah

, Sandberg

, Sereti

: IL-7 treatment supports CD8+ MAIT cell restoration in HIV-1 infected patients on ART. AIDS, 2018; 32:825–828.

10.

Herasimtschuk

, Downey

, Nelson

, et al.: Therapeutic immunisation plus cytokine and hormone therapy improves CD4 T-cell counts, restores anti-HIV-1 responses and reduces immune activation in treated chronic HIV-1 infection. Vaccine, 2014; 32:7005–7013.

11.

Kurioka

, Jahun

, Hannaway

, et al.: Shared and distinct phenotypes and functions of human CD161++ Valpha7.2+ T cell subsets. Front Immunol, 2017; 8:1031.

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Short Communication: Therapeutic Immunization Benefits Mucosal-Associated Invariant T Cell Recovery in Contrast to Interleukin-2,Granulocyte-Macrophage Colony-Stimulating Factor,and Recombinant Human Growth Hormone Addition in HIV-1+ Treated Patients: Individual Case Reports from Phase I Trial

Abstract

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Supplementary Material