IL-15 regulates memory CD8+ T cell O-glycan synthesis and affects trafficking
Jeffrey C. Nolz, John T. Harty
Jeffrey C. Nolz, John T. Harty
Published February 10, 2014
Citation Information: J Clin Invest. 2014;124(3):1013-1026. https://doi.org/10.1172/JCI72039.
View: Text | PDF
Research Article Immunology

IL-15 regulates memory CD8+ T cell O-glycan synthesis and affects trafficking

Abstract

Memory and naive CD8+ T cells exhibit distinct trafficking patterns. Specifically, memory but not naive CD8+ T cells are recruited to inflamed tissues in an antigen-independent manner. However, the molecular mechanisms that regulate memory CD8+ T cell trafficking are largely unknown. Here, using murine models of infection and T cell transfer, we found that memory but not naive CD8+ T cells dynamically regulate expression of core 2 O-glycans, which interact with P- and E-selectins to modulate trafficking to inflamed tissues. Following infection, antigen-specific effector CD8+ T cells strongly expressed core 2 O-glycans, but this glycosylation pattern was lost by most memory CD8+ T cells. After unrelated infection or inflammatory challenge, memory CD8+ T cells synthesized core 2 O-glycans independently of antigen restimulation. The presence of core 2 O-glycans subsequently directed these cells to inflamed tissue. Memory and naive CD8+ T cells exhibited the opposite pattern of epigenetic modifications at the Gcnt1 locus, which encodes the enzyme that initiates core 2 O-glycan synthesis. The open chromatin configuration in memory CD8+ T cells permitted de novo generation of core 2 O-glycans in a TCR-independent, but IL-15–dependent, manner. Thus, IL-15 stimulation promotes antigen-experienced memory CD8+ T cells to generate core 2 O-glycans, which subsequently localize them to inflamed tissues. These findings suggest that CD8+ memory T cell trafficking potentially can be manipulated to improve host defense and immunotherapy.

Authors

Jeffrey C. Nolz, John T. Harty

×

Figure 6

Inflammation is sufficient to generate core 2 O-glycans on circulating memory CD8+ T cells.

Options: View larger image (or click on image) Download as PowerPoint
Inflammation is sufficient to generate core 2 O-glycans on circulating m...
(A) Pre- and post-sort analysis following depletion of memory P14 CD8+ T cells isolated from the spleen that expressed core 2 O-linked glycosylated CD43 (1B11). (B) 1 × 106 1B11lo cells (Thy1.1) from A were transferred into naive B6 mice (Thy1.2) that were then challenged with either saline or CpG. Three days after challenge, memory P14 CD8+ T cells in the lungs were analyzed for the expression of core 2 O-linked glycosylated CD43 (1B11). (C and D) 1 × 106 purified memory P14 CD8+ T cells (Thy1.1) were transferred into naive B6 mice (Thy1.2) followed by intranasal challenge with either saline or CpG. One group of mice received pertussis toxin (Ptx) following CpG challenge. On day 3 after challenge, the number of memory P14 CD8+ T cells in the (C) lung and (D) blood was determined. (E) Expression of core 2 O-linked glycosylated CD43 on memory P14 CD8+ T cells in the lung and blood from C and D. Data are representative of 2 independent experiments, and statistical analysis used 1-way ANOVA with a Bonferroni post-test for multiple comparisons.