MRL/1小鼠颌下炎的免疫组化研究(淋巴细胞增殖和自身免疫)。

H Miyamoto
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摘要

Murphy和Roths报道的MRL/1小鼠是发生单基因突变的狼疮小鼠。他们的特点是表达大量淋巴腺病,脾肿大,关节炎和肾小球肾炎。这些特殊的特征可归因于由常染色体隐性基因控制的异常T细胞的增殖,该基因被称为淋巴增生性(lpr)基因。在本研究中,作者研究了MRL/1小鼠各器官的病理与年龄的关系。探讨MRL/1小鼠自发性上颌下炎的发病机制及发生机制。根据目前对MRL/1小鼠免疫异常的研究,认为颌下炎的发病机制如下:(1) lpr基因的表达导致T细胞增殖并伴有局灶性淋巴细胞浸润;(2)这些增殖的T细胞的辅助T功能诱导多克隆B细胞活化(PBA);(2) PBA导致大量自身抗体和以内源性逆转录病毒糖蛋白为抗原的抗gp70抗体的形成,导致大量免疫复合物的形成;(4)免疫复合物沉积在血管壁上,激活补体系统;(5)诱导中性粒细胞和巨噬细胞浸润;(6)从这些细胞释放的溶酶体酶作为细胞毒性介质起作用并破坏血管壁。总之,颌下炎合并肉芽肿性血管炎可视为由lpr基因遗传决定的免疫异常引起的III型过敏反应;它被认为是免疫复合物疾病的一种亚型。
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[Immunohistochemical study of the submaxillaritis in MRL/1 mouse (lymphoproliferation and autoimmunity)].

MRL/1 mice, reported by Murphy and Roths, are lupus mice in which monogenic mutation has occurred. They are characterized by the expression of massive lymphoadenopathy, splenomegaly, arthritis and glomerulonephritis. These specific characters are attributable to the proliferation of abnormal T cells governed by an autosomal recessive gene, which is called a lymphoproliferative (lpr) gene. In this study, the author has studied the pathology of various organs in MRL/1 mice in relation to their ages. Investigated the pathogenesis of spontaneous submaxillaritis in MRL/1 mice and mechanism of its occurrence. Based on the immunological abnormalities in MRL/1 mice studied thus far, the mechanism of onset of submaxillaritis is believed to be as follows; (1) expression of the lpr gene leads to proliferation of T cells accompanied by focal lymphocyte infiltration in the submandibular gland; (2) the helper T function of these proliferating T cells induces polyclonal B cell activation (PBA); (2) PBA leads to the formation of numerous autoantibodies and anti-gp70 antibody whose antigen is the glycoprotein of endogenous retrovirus, resulting in the massive formation of immune complexes; (4) the immune complexes are deposited on the vascular wall, resulting in activation of the complement system; (5) infiltration of neutrophils and macrophages is induced; and (6) the lysosomal enzymes, released from these cells, effects as a cytotoxic mediator and damages the vascular wall. In brief, submaxillaritis accompanied by granulomatous vasculitis can be regarded as a Type III allergic response caused by immunological abnormalities which are genetically determined by the lpr gene; it is thought to be a subtype of immune complex disease.

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