High pathogen burden in childhood promotes the development of unconventional innate-like CD8+ T cells
Yves T. Falanga, … , Leslie J. Berg, Ann M. Moormann
Yves T. Falanga, … , Leslie J. Berg, Ann M. Moormann
Published August 3, 2017
Citation Information: JCI Insight. 2017;2(15):e93814. https://doi.org/10.1172/jci.insight.93814.
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Research Article Immunology Infectious disease

High pathogen burden in childhood promotes the development of unconventional innate-like CD8+ T cells

Abstract

Cellular and humoral constituents of the immune system differ significantly between children and adults, yet very little is known about the impact of early-life pathogen exposure on this immunologic transition. We examined CD4+ and CD8+ T cell subsets defined by CCR7 and CD45RA expression in two longitudinal pediatric cohorts experiencing divergent levels of pathogen burden. Using multiparameter flow cytometry, along with serological, cytokine, and transcriptomic data, we show that cumulative pathogen burden promotes the development of atypical CD8dim T cells with an innate-like profile (Granzyme Bhi, IFNγlow, TNFαlow, PLFZhi, ID2hi, IKZF2hi) in contrast to age-matched children residing in a low pathogen–exposure area who display a more conventional CD8bright profile (IFNγ+, TNFα+, CCL4+). Furthermore, these unconventional T cells had stunted proliferation, distinct transcriptional programs, and impaired T cell receptor signaling and were enriched in hallmark TNFα, NF-κB, and IL-6 gene signaling pathways, reminiscent of NK cells and type-1 innate lymphoid cells. Our findings suggest that these unconventional CD8dim T cells arise in a very particular immunological context and may provide a deeper understanding of the heterogeneity in human immune responses.

Authors

Yves T. Falanga, Michela Frascoli, Yasin Kaymaz, Catherine Forconi, John Michael Ong’echa, Jeffrey A. Bailey, Leslie J. Berg, Ann M. Moormann

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Figure 4

Healthy African adults have greater proportions of CD3+ CD8dim T cells than healthy North American adults.

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Healthy African adults have greater proportions of CD3+ CD8dim T cells t...
(A) Peripheral blood mononuclear cells (PBMCs) were stained with a panel of fluorescently labeled antibodies to define T cell subsets and then analyzed by multiparameter flow cytometry. Data on the boxplot (median and 95% IQR) display the proportion of CD8dim T cells from healthy Kenyan adults (n = 11) and healthy North American adults (n = 9). Computed two-tailed unpaired t test with Welch’s correction P value is displayed at the bottom of the graph (***P < 0.001). Black dots on the boxplot display values from individual healthy adults. Data generated from 1 flow cytometry experiment. (B) Caspase 3 was detected in ~3% of CD8dim and not in CD8bright T cells, indicating that neither cell population is undergoing apoptosis. (C) Representative flow cytometric analysis of CFSE-labeled profile of CD8bright and CD8dim T cells, either CD45RA+ or CD45RA sorted from the peripheral blood of an adult sample that had previously been exposed to malaria. Cells were analyzed after 72 and 96 hours of stimulation with α-CD3 and α-CD28 antibodies. The number in each plot represents the percentage of cells that proliferated.