Rothe H, Hibino T, Itoh Y, Kolb H, Martin S
Diabetes Research Institute, Heinrich-Heine-University Düsseldorf, Germany.
J Autoimmun. 1997 Jun;10(3):251-6. doi: 10.1006/jaut.1997.0135.
We report that the onset of Th1 insulitis is preceded by a rise of interferon-gamma inducing factor (IGIF) mRNA expression in the spleen. This systemic shift towards Th1 reactivities was underlined by a close correlation of IGIF and IL-12p40 mRNA levels in the spleen, as determined by semi-quantitative RT-PCR. Cyclophosphamide-induced IGIF expression was also observed in MHC congenic NOR mice, but not in MHC class II-incompatible NON mice. The systemic rise of IGIF was followed by the development of destructive Th1-associated intra-insulitis. Interestingly, immunohistochemistry showed IL-4-positive cells evenly dispersed throughout the infiltrate, while IFN-gamma-positive cells were restricted to the vicinity of beta-cells. We conclude that cyclophosphamide induces a systemic shift in antigen presenting cells towards favouring Th1 responses, in an MHC dependent manner. Despite this general bias in immune reactivity, activation of Th1 cells in insulitis occurs only close to beta-cells, indicating a crucial role of antigen presentation by beta-cells or in their immediate vicinity.
我们报告,在脾脏中,干扰素-γ诱导因子(IGIF)mRNA表达升高先于Th1型胰岛炎的发作。半定量逆转录聚合酶链反应(RT-PCR)测定结果显示,脾脏中IGIF和IL-12p40 mRNA水平密切相关,突出了这种向Th1反应性的全身性转变。在MHC同基因NOR小鼠中也观察到环磷酰胺诱导的IGIF表达,但在MHC II类不相容的NON小鼠中未观察到。IGIF的全身性升高之后是与Th1相关的破坏性胰岛内炎的发展。有趣的是,免疫组织化学显示IL-4阳性细胞均匀分布于整个浸润区域,而IFN-γ阳性细胞局限于β细胞附近。我们得出结论,环磷酰胺以MHC依赖的方式诱导抗原呈递细胞发生全身性转变,从而有利于Th1反应。尽管免疫反应存在这种总体偏向,但胰岛炎中Th1细胞的激活仅发生在靠近β细胞的部位,这表明β细胞或其紧邻区域的抗原呈递起着关键作用。
