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白细胞介素-15缺陷型和干扰素调节因子-1缺陷型小鼠胸腺和表皮Vγ3细胞的发育及功能缺陷

Developmental and functional defects of thymic and epidermal V gamma 3 cells in IL-15-deficient and IFN regulatory factor-1-deficient mice.

作者信息

De Creus An, Van Beneden Katrien, Stevenaert Frederik, Debacker Veronique, Plum Jean, Leclercq Georges

机构信息

Department of Clinical Chemistry, Microbiology, and Immunology, University of Ghent, University Hospital, Ghent, Belgium.

出版信息

J Immunol. 2002 Jun 15;168(12):6486-93. doi: 10.4049/jimmunol.168.12.6486.

Abstract

In this study, the role of IL-15 and its regulation by the transcription factor IFN regulatory factor-1 (IRF-1) in murine V gamma 3 T cell development and activity is assessed. Compared with wild-type (WT) mice, reduced numbers of mature V gamma 3 cells were found in the fetal thymus of IL-15(-/-) mice, while IRF-1(-/-) mice displayed normal frequencies. V gamma 3(+) dendritic epidermal T cells (DETCs) were absent in IL-15(-/-) mice but present in IRF-1(-/-) mice. DETCs from IRF-1(-/-) mice displayed morphologically a less mature phenotype and showed different emergence kinetics during ontogeny. This corresponded with lower IL-15 mRNA levels in the skin epidermis. Comparable levels of IL-7 were found in the skin of WT and IL-15(-/-) mice. Adoptive transfer experiments of WT fetal thymocytes into IL-15(-/-) mice did not result in the development of V gamma 3(+) DETCs, confirming the nonredundant role of IL-15 in the skin during DETC development. In vitro, cytolytic activity of IL-15(-/-) V gamma 3 cells was normal after stimulation with IL-15 and was further enhanced by addition of IL-12. In contrast, cytolytic activity of IRF-1(-/-) V gamma 3 cells remained defective after stimulation with IL-15 in combination with IL-12. These data suggest that IL-15 is redundant for the development and/or survival of mature V gamma 3 cells in the fetal thymus, whereas it is essential for the localization of V gamma 3 cells in the skin. Furthermore, a possible role for IRF-1 in inducing morphological maturation of DETCs and cytolytic capacity of V gamma 3 cells is suggested.

摘要

在本研究中,评估了白细胞介素-15(IL-15)的作用及其受转录因子干扰素调节因子-1(IRF-1)调控在小鼠Vγ3 T细胞发育和活性中的作用。与野生型(WT)小鼠相比,在IL-15基因敲除(-/-)小鼠的胎儿胸腺中发现成熟Vγ3细胞数量减少,而IRF-1基因敲除(-/-)小鼠的频率正常。IL-15基因敲除(-/-)小鼠中不存在Vγ3(+)树突状表皮T细胞(DETC),但在IRF-1基因敲除(-/-)小鼠中存在。来自IRF-1基因敲除(-/-)小鼠的DETC在形态上表现出不太成熟的表型,并且在个体发育过程中显示出不同的出现动力学。这与皮肤表皮中较低的IL-15 mRNA水平相对应。在WT和IL-15基因敲除(-/-)小鼠的皮肤中发现了相当水平的IL-7。将WT胎儿胸腺细胞过继转移到IL-15基因敲除(-/-)小鼠中并未导致Vγ3(+)DETC的发育,证实了IL-15在皮肤中DETC发育过程中的非冗余作用。在体外,IL-15基因敲除(-/-)的Vγ3细胞在用IL-15刺激后细胞溶解活性正常,并且通过添加IL-12进一步增强。相比之下,IRF-1基因敲除(-/-)的Vγ3细胞在用IL-15和IL-12联合刺激后细胞溶解活性仍然存在缺陷。这些数据表明,IL-15对于胎儿胸腺中成熟Vγ3细胞的发育和/或存活是冗余的,而对于Vγ3细胞在皮肤中的定位是必不可少的。此外,提示了IRF-1在诱导DETC形态成熟和Vγ3细胞细胞溶解能力方面可能发挥的作用。

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