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自发性糖尿病Bio Breeding/Worcester(BB/W)大鼠的实验研究——特别提及大鼠主要组织相容性复合体(RT1)在该疾病发展中的作用

[An experimental study of spontaneously diabetic Bio Breeding/Worcester (BB/W) rats--with special references to the rat MHC (RT1) in the development of the disease].

作者信息

Misonou J

机构信息

First Department of Pathology, Hokkaido University School of Medicine, Sapporo, Japan.

出版信息

Hokkaido Igaku Zasshi. 1989 May;64(3):349-62.

PMID:2570014
Abstract

The role of rat MHC (RT1) in the development of diabetes mellitus was studied on the Bio Breeding/Worcester (BB/W) rat, an experimental model animal for human juvenile onset (Insulin-dependent, Type 1) diabetes mellitus. The rate of the development of diabetes mellitus was as follows; 35/45 (77.8%) in inbred BB/W rats (u/u haplotype), and 5/397 (1.7%) in F2 rats. Histopathological examinations demonstrated that there were lymphocytic thyroiditis, T cell depletion in the spleen and in the lymph nodes, and extramedullary hematopoiesis, in addition to typical lymphocytic insulitis in the pancreas. Immunohistochemically, the expression of class II antigens in the pancreas was shown to be highly concerned with the histopathological changes and the clinical onset of the diabetes mellitus. Analysis of subsets of infiltrating cells demonstrated that macrophages appeared in the pancreas prior to the onset of the disease. And it was suggested that the infiltrated OX 6+ macrophages functioned as antigen presenting cells, leading to expression of the class II antigens on the surface of islet cells, and finally caused severe lymphocytic insulitis. However, BB/W rats showed complete negative immunohistochemical stainings with a monoclonal antibody HOK 2B, which stained other rat strains carrying RT1u class II antigen (TO, SDJ). Moreover, differences in blocking effect of HOK 2B were found on mixed lymphocyte reactions (MLR) between BB/W and other strains with RT1u haplotype. These findings raise the possibility that minor heterogeneities exist in the structure of class II molecules in RT1u rats including BB/W, which might be closely related to the onset of the disease.

摘要

在生物繁殖/伍斯特(BB/W)大鼠(一种人类青少年发病型(胰岛素依赖型,1型)糖尿病的实验模型动物)上研究了大鼠主要组织相容性复合体(RT1)在糖尿病发展中的作用。糖尿病的发展速率如下:近交系BB/W大鼠(u/u单倍型)中为35/45(77.8%),F2大鼠中为5/397(1.7%)。组织病理学检查表明,除胰腺中典型的淋巴细胞性胰岛炎外,还有淋巴细胞性甲状腺炎、脾脏和淋巴结中的T细胞耗竭以及髓外造血。免疫组织化学显示,胰腺中II类抗原的表达与糖尿病的组织病理学变化和临床发病高度相关。对浸润细胞亚群的分析表明,巨噬细胞在疾病发作前出现在胰腺中。并且提示浸润的OX 6+巨噬细胞作为抗原呈递细胞发挥作用,导致胰岛细胞表面II类抗原的表达,最终引起严重的淋巴细胞性胰岛炎。然而,BB/W大鼠用单克隆抗体HOK 2B进行免疫组织化学染色完全呈阴性,该抗体可对携带RT1u II类抗原的其他大鼠品系(TO、SDJ)进行染色。此外,还发现HOK 2B对BB/W大鼠和其他具有RT1u单倍型的品系之间的混合淋巴细胞反应(MLR)的阻断作用存在差异。这些发现增加了一种可能性,即在包括BB/W在内的RT1u大鼠中,II类分子结构存在微小异质性,这可能与疾病的发生密切相关。

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