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突变型糖尿病(db/db)小鼠的胸腺功能障碍。

Thymic dysfunction in the mutant diabetic (db/db) mouse.

作者信息

Dardenne M, Savino W, Gastinel L N, Nabarra B, Bach J F

出版信息

J Immunol. 1983 Mar;130(3):1195-9.

PMID:6571875
Abstract

Thymic function has been explored in genetically diabetic homozygous C57BL/KsJ (db/db) mice by evaluating their serum thymic factor (FTS) levels with a rosette assay. As previously reported for other autoimmune mice (NZB or MRL/I mice), the age-dependent decline of FTS levels was significantly accelerated in diabetic mice when compared to heterozygous littermates. Furthermore, FTS inhibitory molecules were detected in db/db mouse sera (as early as 10 wk of age) as evaluated by their ability to absorb in vitro the activity of synthetic FTS in the rosette assay, and in vivo for their capacity to induce the disappearance of endogenous FTS when injected into normal mice. These inhibitors were shown to be immunoglobulins. Histologically, the thymus presented an accelerated involution starting with a cortical lymphocytic depletion and an increased number of Hassall's corpuscles. Ultrastructural studies showed alterations in thymic epithelial cells, mainly represented by an increasing number of cytoplasmic vacuoles. By means of indirect immunofluorescence with anti-FTS monoclonal antibodies, it was shown that the number of FTS+ cells was reduced in db/db mouse thymuses: at the age of 22 wk, diabetic mice had 10 times fewer FTS+ cells than heterozygotes of the same age. Taken together, these results indicate important abnormalities in the thymus of diabetic mice. It is possible that the associated lymphocyte dysfunction plays a role in the pathogenesis of the autoimmune disease presented by db/db mice.

摘要

通过玫瑰花结试验评估遗传性糖尿病纯合子C57BL/KsJ(db/db)小鼠的血清胸腺因子(FTS)水平,对其胸腺功能进行了研究。正如之前针对其他自身免疫性小鼠(NZB或MRL/I小鼠)所报道的那样,与杂合子同窝小鼠相比,糖尿病小鼠中FTS水平随年龄的下降明显加速。此外,通过玫瑰花结试验评估db/db小鼠血清中FTS抑制分子在体外吸收合成FTS活性的能力,并在体内评估其注射到正常小鼠中诱导内源性FTS消失的能力,结果发现这些抑制分子在db/db小鼠血清中(最早在10周龄时)即可检测到。这些抑制剂被证明是免疫球蛋白。组织学上,胸腺呈现出加速退化,始于皮质淋巴细胞耗竭和哈氏小体数量增加。超微结构研究显示胸腺上皮细胞发生改变,主要表现为细胞质空泡数量增加。通过用抗FTS单克隆抗体进行间接免疫荧光检测,发现db/db小鼠胸腺中FTS+细胞数量减少:在22周龄时,糖尿病小鼠的FTS+细胞数量比同年龄杂合子少10倍。综上所述,这些结果表明糖尿病小鼠胸腺存在重要异常。相关的淋巴细胞功能障碍可能在db/db小鼠所呈现的自身免疫性疾病发病机制中起作用。

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