Cyclic adenosine monophosphate (cAMP) differentially regulates IL-4 in thymocyte subsets.

Thymus Pub Date : 1996-01-01
S Wirth, M Lacour, F Jaunin, C Hauser
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Abstract

It was recently reported that cAMP upregulated IL-4 in T cell lines generated in vitro and expressing an unrestricted lymphokine pattern. In order to study the effect of cAMP on IL-4 released by freshly isolated T cell populations, we tested various T cell subsets that have previously been reported to synthesize this lymphokine. We found that cAMP upregulated IL-4 release from in vivo activated single CD4+ peripheral T cells and CD4+CD8-HSAlowNK1.1- thymocytes stimulated with ionomycin and phorbol ester. Furthermore, as in conventional single CD4+ or CD8+ thymocytes, cAMP enhanced IL-4 production in CD4+CD8-NK1.1+ thymocytes. This latter subset has recently been shown to belong to a independent T cell lineage that is positively selected by MHC class I molecules, recognizes CD1 and expresses a restricted T cell receptor repertoire. In contrast, cAMP appeared not to upregulate IL-4 in a third independent T cell lineage. This was suggested by the observation that cAMP did not increase IL-4 in CD3+CD4-CD8- thymocytes, which are thought not to give rise to conventional single CD4+ or CD8+ T cells. It therefore appears that cAMP is coupled differently to IL-4, depending on the T cell lineage. In contrast, in all IL-4 producing stages of conventional T cells, IL-4 is consistently upregulated by cAMP.

环磷酸腺苷(cAMP)在胸腺细胞亚群中调控IL-4的差异。
最近有报道称,cAMP在体外生成的表达不受限制的淋巴因子模式的T细胞系中上调IL-4。为了研究cAMP对新分离的T细胞群释放的IL-4的影响,我们测试了先前报道的合成这种淋巴因子的各种T细胞亚群。我们发现cAMP上调了体内活化的单个CD4+外周T细胞和受离子霉素和磷酯刺激的CD4+CD8-HSAlowNK1.1-胸腺细胞的IL-4释放。此外,与传统的单个CD4+或CD8+胸腺细胞一样,cAMP增强了CD4+CD8- nk1.1 +胸腺细胞中IL-4的产生。后一个亚群最近被证明属于一个独立的T细胞谱系,它被MHC I类分子积极选择,识别CD1并表达一个受限的T细胞受体库。相反,在第三个独立的T细胞谱系中,cAMP似乎没有上调IL-4。观察结果表明,cAMP不会增加CD3+CD4-CD8-胸腺细胞中的IL-4,这被认为不会产生传统的单个CD4+或CD8+ T细胞。因此,cAMP似乎与IL-4的偶联方式不同,这取决于T细胞谱系。相反,在常规T细胞产生IL-4的所有阶段,IL-4都被cAMP持续上调。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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