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糖尿病与新西兰肥胖(NZO)小鼠的自身免疫有关。

Diabetes is associated with autoimmunity in the New Zealand obese (NZO) mouse.

作者信息

Melez K A, Harrison L C, Gilliam J N, Steinberg A D

出版信息

Diabetes. 1980 Oct;29(10):835-40. doi: 10.2337/diacare.20.10.835.

Abstract

The New Zealand Obese (NZO) mouse was studied as a potential model for autoimmune diabetes. NZO mice develop obesity, glucose intolerance, and insulin resistance, and have low-titer IgM antibodies to the insulin receptor. It is shown that they have circulating antibodies to both native DNA and denatured, single-stranded DNA. The antibody levels are higher in females, and, up to 6 mo of age, are comparable to those found in the related NZB X NZW F1 (NZB/W) mouse, a model for systemic lupus erythematosus. After 6 mo of age the antibody levels in NZO mice fall toward normal, in contrast to the persistently elevated levels in NZB/W mice. NZB/W mice are known to succumb to immune complex-mediated proliferative glomerulonephritis before 1 yr of age, whereas NZO mice survive. NZO kidneys exhibit light microscopic features of both diabetic and lupus nephropathies: glomerular proliferation, mesangial deposits, mild basement membrane thickening, glomerulosclerosis, eosinophilic nodules in some glomeruli, occasional hyalinization of the glomerular arterioles, and healing arteriolar inflammation. These changes are associated with glomerular deposition of immunoglobulin, especially IgM, in a granular pattern on fluorescent staining. The NZO mouse, therefore, has evidence of a generalized immune disorder and provides a model for studying the relationship between autoimmunity, obesity, and diabetes.

摘要

新西兰肥胖(NZO)小鼠被作为自身免疫性糖尿病的潜在模型进行研究。NZO小鼠会出现肥胖、葡萄糖不耐受和胰岛素抵抗,并且对胰岛素受体有低滴度的IgM抗体。研究表明,它们对天然DNA和变性单链DNA都有循环抗体。抗体水平在雌性中更高,并且在6月龄之前,与相关的新西兰黑鼠X新西兰白鼠F1(NZB/W)小鼠(一种系统性红斑狼疮模型)中的抗体水平相当。6月龄后,NZO小鼠的抗体水平降至正常,而NZB/W小鼠的抗体水平则持续升高。已知NZB/W小鼠在1岁前会死于免疫复合物介导的增殖性肾小球肾炎,而NZO小鼠存活下来。NZO小鼠的肾脏表现出糖尿病性和狼疮性肾病的光学显微镜特征:肾小球增殖、系膜沉积物、轻度基底膜增厚、肾小球硬化、一些肾小球中的嗜酸性结节、偶尔的肾小球小动脉玻璃样变以及愈合的小动脉炎症。这些变化与免疫球蛋白(尤其是IgM)在荧光染色下呈颗粒状模式的肾小球沉积有关。因此,NZO小鼠有全身性免疫紊乱的证据,并为研究自身免疫、肥胖和糖尿病之间关系提供了一个模型。

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