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 Syndrome Toxin-1 than Cord Blood CD4+ T Cells

Author:

Imanishi Ken’ichi1,Seo Kazuhiro2,Kato Hidehito1,Miyoshi-Akiyama Tohru1,Zhang Rui-Hua1,Takanashi Yoshinori2,Imai Yasuharu2,Uchiyama Takehiko134

Affiliation:

1. *Department of Microbiology and Immunology,

2. §Department of Pediatric Cardiovascular Surgery, The Heart Institute of Japan, Tokyo Women’s Medical College, Tokyo, Japan

3. †Department of Infectious Disease Control,

4. ‡Institute of Laboratory Animals, and

Abstract

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.

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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