CD45-mediated control of TCR tuning in naïve and memory CD8+ T cells

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Abstract

Continuous contact with self-major histocompatibility complex (MHC) ligands is essential for survival of naïve T cells but not memory cells. This surprising finding implies that T cell subsets may vary in their relative T-cell receptor (TCR) sensitivity. Here we show that in CD8+ T cells TCR sensitivity correlates inversely with levels of CD5, a marker for strong self-MHC reactivity. We also show that TCR sensitivity is lower in memory CD8+ T cells than naïve cells. In both situations, TCR hypo-responsiveness applies only to short-term TCR signalling events and not to proliferation, and correlates directly with increased expression of a phosphatase, CD45 and reciprocal decreased expression of activated LCK. Inhibition by high CD45 on CD8+ T cells may protect against overt TCR auto-MHC reactivity, while enhanced sensitivity to cytokines ensures strong responses to foreign antigens.

Figures

  • Fig. 3. (b) Levels of miR181a (mean  s.d.) and mRNA for the indicated phosphatases in B6 CD44lo CD5lo and CD5hi and CD44hi CD8+ T cells. (c) ERK phosphorylation in CD44lo B6 naïve CD8+ T cells after incubation with S-CD3 mAb  titrated concentrations of the indicated inhibitors; their specificity for a variety of phosphatases is described in Methods section. Data are representative of three (a,c) and five independent experiments (b). Unpaired Student’s t-test was used for the statistical analysis. *, P < 0.05; **, P < 0.0005; ns, not significant.

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CITATION STYLE

APA

Cho, J. H., Kim, H. O., Ju, Y. J., Kye, Y. C., Lee, G. W., Lee, S. W., … Sprent, J. (2016). CD45-mediated control of TCR tuning in naïve and memory CD8+ T cells. Nature Communications, 7. https://doi.org/10.1038/ncomms13373

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