Sobel Douglas O, Han Jaeseok, Williams Joy, Yoon Ji-Won, Jun Hee-Sook, Ahvazi Behrouz
Georgetown University Medical Center, Division of Pediatric Endocrinology and Metabolism, 3800 Reservoir Road N.W., 2 PHC, Washington, DC 20007-2197, USA.
J Autoimmun. 2002 Nov;19(3):129-37. doi: 10.1006/jaut.2002.0604.
Gamma interferon (IFN-gamma) has been thought to play an important role in the pathogenesis of diabetes. This report determines if rIFN-gamma administration to NOD mice paradoxically inhibits the development of diabetes. Injections of recombinant rIFN-gamma of 5 x 10(3), 20 x 10(3), and 100 x 10(3) units, dose dependently inhibited the development of diabetes. The maximal rIFN-gamma dose decreased the incidence of diabetes from 74% in control animals to 42%. 100x10(3) unit rIFN-gamma dose significantly decreased insulitis score, and increased islet number. The development of diabetes in irradiated NOD mice was slower in animals injected with spleen cells from rIFN-gamma treated than from saline treated NOD mice suggesting that rIFN-gamma decreases anti-islet effector cell activity. The susceptibility to apoptosis was increased in splenic cells of rIFN-gamma treated mice. The expressions of the co-stimulatory molecules B7-2 and ICAM-1 were significantly increased in spleen cells of rIFN-gamma treated mice while the expression of MHC class I was decreased. In vitro studies demonstrated that NOD mouse mononuclear spleen cells preincubated with rIFN-gamma and subsequently cocultured with responder cells, potently inhibited responder T-cell proliferative responses. rIFN-gamma administration decreased IL-12 and IL-2 mRNA expression in spleen cells while increasing IL-1 expression. In conclusion, rIFN-gamma inhibits the diabetic process in NOD mice by decreasing anti-islet effector activity and in turn decreasing insulitis and islet destruction. The suppression of Th1 cell related cytokines and/or augmentation of the macrophage cytokine IL-1 may play a role in the diabetes sparing effect of rIFN-gamma.
γ干扰素(IFN-γ)被认为在糖尿病发病机制中起重要作用。本报告旨在确定向非肥胖糖尿病(NOD)小鼠注射重组IFN-γ(rIFN-γ)是否会反常地抑制糖尿病的发展。注射5×10³、20×10³和100×10³单位的重组rIFN-γ,剂量依赖性地抑制了糖尿病的发展。最大剂量的rIFN-γ将糖尿病发病率从对照动物的74%降至42%。100×10³单位的rIFN-γ剂量显著降低了胰岛炎评分,并增加了胰岛数量。在接受照射的NOD小鼠中,注射经rIFN-γ处理的小鼠脾细胞的动物,其糖尿病发展比注射生理盐水处理的NOD小鼠脾细胞的动物更慢,这表明rIFN-γ降低了抗胰岛效应细胞的活性。rIFN-γ处理的小鼠脾细胞对凋亡的敏感性增加。rIFN-γ处理的小鼠脾细胞中,共刺激分子B7-2和细胞间黏附分子-1(ICAM-1)的表达显著增加,而主要组织相容性复合体I类(MHC class I)的表达则降低。体外研究表明,预先用rIFN-γ孵育的NOD小鼠单核脾细胞,随后与反应细胞共培养,能有效抑制反应性T细胞的增殖反应。给予rIFN-γ可降低脾细胞中白细胞介素-12(IL-12)和白细胞介素-2(IL-2)mRNA的表达,同时增加白细胞介素-1(IL-1)的表达。总之,rIFN-γ通过降低抗胰岛效应活性,进而减少胰岛炎和胰岛破坏,抑制NOD小鼠的糖尿病进程。抑制Th1细胞相关细胞因子和/或增强巨噬细胞细胞因子IL-1可能在rIFN-γ的糖尿病缓解作用中发挥作用。
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