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Mls-1a小鼠个体发育过程中自身反应性成熟和未成熟T细胞的激活与“清除”:对新生儿耐受性诱导的影响

Activation and 'deletion' of self-reactive mature and immature T cells during ontogeny of Mls-1a mice: implications for neonatal tolerance induction.

作者信息

Marodon G, Rocha B

机构信息

INSERM U345, CNRS UA122, Institut Necker, Paris, France.

出版信息

Int Immunol. 1994 Dec;6(12):1899-904. doi: 10.1093/intimm/6.12.1899.

Abstract

We assessed the kinetics of V beta 6+ T cell elimination in the lymph nodes and thymus during Mls-1a mouse ontogeny. Our results suggest that induction of tolerance to Mls-1a antigens involves mechanisms other than clonal deletion of immature T cells in the thymus. Mature CD4+CD8- (CD4SP) T cells were affected by Mls-1a antigens earlier than immature thymocyte populations. Up to 2 weeks after birth, reduced frequencies of V beta 6+ T cells were detected only in CD4SP cells from the thymus and lymph nodes, and generation of CD4SP cells in the thymus was blocked at least 1 week earlier than that of their CD4+CD8loTCRhi immature precursors. The number of V beta 6+CD4SP T cells increased during the first 2 weeks of life and remained constant thereafter. We thus found no evidence of deletion of mature V beta 6+CD4SP T cells, as the reduced frequencies in adult mice can be attributed to the dilution of previously generated cells in lymphoid organs of growing mice, which increase in cellularity after birth. V beta 6+CD4+ T cells were activated in vivo shortly after birth, as shown by a selective increase in IL-2 receptor alpha chain expression in the thymus and lymph nodes from day 0 to day 2 after birth. It is therefore likely that endogenous expression of Mls-1a antigen shortly after birth activates V beta 6+CD4SP T cells and renders them anergic. This process of tolerance induction may precede the clonal deletion of immature T cells in the thymus, described in the adult mouse.

摘要

我们评估了Mls-1a小鼠个体发育过程中淋巴结和胸腺中Vβ6 + T细胞清除的动力学。我们的结果表明,对Mls-1a抗原的耐受性诱导涉及胸腺中未成熟T细胞克隆清除以外的机制。成熟的CD4 + CD8-(CD4SP)T细胞比未成熟的胸腺细胞群体更早受到Mls-1a抗原的影响。出生后长达2周,仅在胸腺和淋巴结的CD4SP细胞中检测到Vβ6 + T细胞频率降低,并且胸腺中CD4SP细胞的产生比其CD4 + CD8loTCRhi未成熟前体至少提前1周受阻。Vβ6 + CD4SP T细胞的数量在生命的前2周内增加,此后保持恒定。因此,我们没有发现成熟的Vβ6 + CD4SP T细胞被清除的证据,因为成年小鼠中频率降低可归因于生长小鼠淋巴器官中先前产生的细胞的稀释,出生后细胞数量增加。出生后不久,Vβ6 + CD4 + T细胞在体内被激活,从出生后第0天到第2天,胸腺和淋巴结中IL-2受体α链表达的选择性增加表明了这一点。因此,出生后不久Mls-1a抗原的内源性表达可能激活Vβ6 + CD4SP T细胞并使其无反应。这种耐受性诱导过程可能先于成年小鼠中描述的胸腺中未成熟T细胞的克隆清除。

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