Impaired survival and proliferation in IL-7 receptor-deficient peripheral T cells.

生物 T细胞 白细胞介素21 细胞毒性T细胞 离子霉素 CD8型 白细胞介素3 分子生物学 细胞生物学 白细胞介素2受体 免疫学 体外 刺激 抗原 免疫系统 内分泌学 生物化学
作者
Eugene Maraskovsky,Mark Teepe,P J Morrissey,Steve Braddy,Robert E. Miller,David H. Lynch,Jacques J. Peschon
出处
期刊:Journal of Immunology [The American Association of Immunologists]
卷期号:157 (12): 5315-5323 被引量:133
标识
DOI:10.4049/jimmunol.157.12.5315
摘要

Mice genetically deficient in IL-7R(alpha) are highly lymphopenic in the peripheral lymphoid organs. The functional competence of T cells that have developed in the absence of an IL-7R signal was investigated. Three important observations were made using several in vitro activation regimens. First, stimulation of T cells from IL-7R -/- mice at limiting dilution with immobilized Abs to CD3, CD4 or CD8, and CD18 revealed a six- to sevenfold reduction in the frequency of clonogenic T cells compared with T cells from IL-7R +/+ mice. IL-7R -/- T cells were also significantly less responsive to alloantigen as well as to receptor-independent stimuli such as PMA and ionomycin. Furthermore, the average clone size of single IL-7R -/- T cells was 50% smaller than that of IL-7R +/+ T cells. These data suggest that the reduced clonogenicity was predominantly due to intrinsic deficiencies in the ability of IL-7R -/- T cells to proliferate upon stimulation. Second, analysis of the kinetics of cell growth of IL-7R -/- T cells revealed that a significant proportion of T cells failed to proliferate within the first 72 h of in vitro stimulation, with the majority undergoing programmed cell death. Third, both clonogenic IL-7 -/- T cells and IL-7R +/+ T cells showed a similar proliferative response in the presence of IL-2 and similar survival kinetics, indicating that a subpopulation of IL-7R -/- T cells is functionally mature. We propose that an absence of IL-7R signaling not only affects T cell development in the thymus, but also results in the accumulation of functionally inactive T cells in the periphery.
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