Post-thymic maturation of migrating human thymic single-positive T cells: thymic CD1a− CD4+ T cells are more susceptible to anergy induction by toxic shock …

K Imanishi, K Seo, H Kato… - The Journal of …, 1998 - journals.aai.org
K Imanishi, K Seo, H Kato, T Miyoshi-Akiyama, RH Zhang, Y Takanashi, Y Imai, T Uchiyama
The Journal of Immunology, 1998journals.aai.org
To determine whether human CD4+ T cells undergo post-thymic maturation, we compared
the susceptibility to anergy induction in human thymic CD1a− CD4+ single-positive (CD4+),
cord blood (CB) CD4+, and adult peripheral blood (APB) CD4+ T cells by stimulation with
toxic shock syndrome toxin-1 (TSST-1). Most TSST-1-induced T cell blasts derived from
either T cell preparation expressed TCR Vβ2, which determines the potential reactivity to
TSST-1. Most thymic CD4+ T cell blast preparations exhibited little or no production of IL-2 …
Abstract
To determine whether human CD4+ T cells undergo post-thymic maturation, we compared the susceptibility to anergy induction in human thymic CD1a− CD4+ single-positive (CD4+), cord blood (CB) CD4+, and adult peripheral blood (APB) CD4+ T cells by stimulation with toxic shock syndrome toxin-1 (TSST-1). Most TSST-1-induced T cell blasts derived from either T cell preparation expressed TCR Vβ2, which determines the potential reactivity to TSST-1. Most thymic CD4+ T cell blast preparations exhibited little or no production of IL-2 and IL-4 after restimulation with TSST-1 and only marginal responses after stimulation with rIL-2 or a combination of PMA and calcium ionophore, while the APB CD4+ T cell blasts showed high responses to these stimuli. The responses of CB CD4+ T cell blasts to these stimuli varied, ranging from minimal to relatively high. Studies of DNA fragmentation showed that there was no significant cell death of thymic CD4+ T cell blasts. Most thymic CD1a− CD4+ and CB CD4+ T cells were CD38 positive. APB CD4+ T cell blasts derived from the CD38+ fraction and from the CD38− fraction exhibited equally high responses to restimulation with TSST-1. These results indicate that thymic CD1a− CD4+ and CB CD4+ T cells are inherently highly susceptible to anergy induction by bacterial superantigens and that thymic CD1a− CD4+ T cells are less mature than CB CD4+ T cells, suggesting that post-thymic maturation in thymic T cells migrating to the periphery is required for acquisition of full reactivity to antigenic stimulation.
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