Baek H S, Yoon J W
Laboratory of Viral and Immunopathogenesis of Diabetes, Julia McFarlane Diabetes Research Centre, University of Calgary, Alberta, Canada.
Diabetes. 1991 Dec;40(12):1586-97. doi: 10.2337/diab.40.12.1586.
A single administration of complete Freund's adjuvant (CFA), type 1 carrageenan (Car), or silica 7, 2, and 2 days, respectively, before infection with a low dose (1 x 10(2) plaque-forming units/mouse) of encephalomyocarditis D (EMC-D) virus resulted in a significant increase in the incidence of diabetes in SJL/J mice (100%) compared with untreated EMC-D virus-infected mice (40%). Peritoneal macrophages were isolated from uninfected SJL/J mice, which had been treated once with silica, and transferred into SJL/J mice 2 days before low-dose EMC-D infection. Approximately 90% of the mice became diabetic, whereas 30% of mice that received virus alone became diabetic. The depletion of macrophages by treatment with the combined anti-Mac-1 and anti-Mac-2 monoclonal antibodies after a single administration of CFA, Car, or silica resulted in almost complete prevention of beta-cell destruction in EMC-D virus-infected mice. Furthermore, none of the mice in which macrophages were depleted by long-term treatment with silica and 10% of the mice treated with Car before virus infection became diabetic. On the basis of these observations, we conclude that macrophages are directly involved in the destruction of beta-cells, leading to the development of clinical diabetes in EMC-D virus-infected mice.
在感染低剂量(1×10² 蚀斑形成单位/小鼠)脑心肌炎D(EMC-D)病毒前7天、2天和2天分别单次给予完全弗氏佐剂(CFA)、I型角叉菜胶(Car)或二氧化硅,结果显示与未处理的EMC-D病毒感染小鼠(40%)相比,SJL/J小鼠的糖尿病发病率显著增加(100%)。从未感染的SJL/J小鼠中分离出腹膜巨噬细胞,这些小鼠曾用二氧化硅处理过一次,并在低剂量EMC-D感染前2天转移到SJL/J小鼠体内。大约90%的小鼠患糖尿病,而仅接受病毒感染的小鼠中30%患糖尿病。在单次给予CFA、Car或二氧化硅后,用抗Mac-1和抗Mac-2单克隆抗体联合处理以耗尽巨噬细胞,几乎完全预防了EMC-D病毒感染小鼠的β细胞破坏。此外,长期用二氧化硅处理使巨噬细胞耗尽的小鼠以及在病毒感染前用Car处理的小鼠中,均无小鼠患糖尿病。基于这些观察结果,我们得出结论,巨噬细胞直接参与β细胞的破坏,导致EMC-D病毒感染小鼠发生临床糖尿病。
