Differential localization and limited cytotoxic potential of duodenal CD8+ T cells
Leonard Mvaya, Trevor Khaba, Agness E. Lakudzala, Thandeka Nkosi, Ndaru Jambo, Innocent Kadwala, Anstead Kankwatira, Priyanka D. Patel, Melita A. Gordon, Tonney S. Nyirenda, Kondwani C. Jambo, Zaza M. Ndhlovu
Leonard Mvaya, Trevor Khaba, Agness E. Lakudzala, Thandeka Nkosi, Ndaru Jambo, Innocent Kadwala, Anstead Kankwatira, Priyanka D. Patel, Melita A. Gordon, Tonney S. Nyirenda, Kondwani C. Jambo, Zaza M. Ndhlovu
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Research Article AIDS/HIV Immunology

Differential localization and limited cytotoxic potential of duodenal CD8+ T cells

Abstract

The duodenum is a major site of HIV persistence during suppressive antiretroviral therapy despite harboring abundant tissue-resident memory (Trm) CD8+ T cells. The role of duodenal Trm CD8+ T cells in viral control is still not well defined. We examined the spatial localization, phenotype, and function of CD8+ T cells in the human duodenal tissue from people living with HIV (PLHIV) and healthy controls. We found that Trm (CD69+CD103hi) cells were the predominant CD8+ T cell population in the duodenum. Immunofluorescence imaging of the duodenal tissue revealed that CD103+CD8+ T cells were localized in the intraepithelial region, while CD103–CD8+ T cells and CD4+ T cells were mostly localized in the lamina propria (LP). Furthermore, HIV-specific CD8+ T cells were enriched in the CD69+CD103–/lo population. However, the duodenal HIV-specific CD8+ Trm cells rarely expressed canonical molecules for potent cytolytic function (perforin and granzyme B) but were more polyfunctional than those from peripheral blood. Taken together, our results show that duodenal CD8+ Trm cells possess limited perforin-mediated cytolytic potential and are spatially separated from HIV-susceptible LP CD4+ T cells. This could contribute to HIV persistence in the duodenum and provides critical information for the design of cure therapies.

Authors

Leonard Mvaya, Trevor Khaba, Agness E. Lakudzala, Thandeka Nkosi, Ndaru Jambo, Innocent Kadwala, Anstead Kankwatira, Priyanka D. Patel, Melita A. Gordon, Tonney S. Nyirenda, Kondwani C. Jambo, Zaza M. Ndhlovu

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Figure 3

Characterization of cytotoxic potential of duodenal and peripheral blood CD8+ T cells.

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Characterization of cytotoxic potential of duodenal and peripheral blood...
Unstimulated DMNCs and PBMCs from HIV-uninfected adults and PLHIV were stained with fluorochrome-conjugated antibodies against surface markers of interest. Intracellular staining was done to detect preformed perforin and granzyme B within CD8+ T cells. (A) Comparison of preformed perforin and granzyme B expression by duodenal and peripheral blood CD8+ T cells in a collated group of HIV-uninfected individuals and PLHIV (HIV−, n = 9; ART, n = 13; ART+, n = 10). (B) Representative flow cytometry plots showing preformed perforin and granzyme B expression in unstimulated Trm and CD69+CD103–/lo duodenal CD8+ T cells from a healthy control. (C) Comparison of preformed perforin and granzyme B expression by Trm and CD69+CD103–/lo CD8+ T cells in a collated group of HIV-uninfected individuals and PLHIV (HIV−, n = 12; ART, n = 13; ART+, n = 10). Data were analyzed using repeated measures 1-way ANOVA test (A, C). (D) Association between CD103 and granzyme B expression in bulk duodenal CD8+ T cells from all study participant groups (HIV−, n = 12; ART, n = 13; ART+, n = 10). Data were analyzed using Pearson’s correlation test. (E) Representative IHC image of duodenal biopsy section showing granzyme B (red), CD103 (yellow), CD8 (green), and DAPI (blue) staining. (F) Density of duodenal mucosa granzyme B expressing CD8+ T cells, which are either CD103+ or CD103. Data were analyzed using Mann–Whitney test.