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Hamartin and Tuberin Expression in Human Tissues

机译:Hamartin和Tuberin在人体组织中的表达

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Tuberous sclerosis (TSC) is a bigenic autosomal dominant disease caused by mutations in one of two tumor-suppressor genes, TSC1 and TSC2, resulting in benign hamartomas and low grade neoplasms in multiple organs including brain, heart, kidney, and skin. We report the results of an immunohistochemical study of the expression of the TSC gene products, tuberin and hamartin, in multiple tissues obtained at autopsy from 12 non-TSC affected patients ranging in age from 20 weeks gestation to 8 years, and surgical specimens from some organs. Tuberin and hamartin are expressed and are colocalized in most tissues. Contrary to a previous report, immunostaining with our antisera detected hamartin in liver, small and large intestine, prostate, and testes. We did not detect significant developmental differences in tuberin or hamartin expression in comparable tissues from patients of different ages. Although tuberin and hamartin colocalize in most tissues and cell types, we provide data that hamartin is more abundantly expressed than tuberin in cells within some tissues including the distal nephron and a population of cells of the endocrine pancreas. These data support the hypothesis that hamartin and tuberin interact and may function together in many tissues where they are co-expressed, but also suggest that hamartin has a discrete and specialized function in certain cell types.
机译:结节性硬化症(TSC)是一种双基因常染色体显性遗传疾病,由两个肿瘤抑制基因TSC1和TSC2中的一个突变引起,导致良性错构瘤和低级肿瘤在包括大脑,心脏,肾脏和皮肤在内的多个器官中发生。我们报告了免疫组织化学研究的结果,该研究是在从20孕周至8岁不等的12例非TSC感染患者的尸体解剖中获得的,在多个组织中对TSC基因产物,结核菌素和hamartin的表达以及一些外科标本的表达的器官。 Tuberin和hamartin在大多数组织中表达并共定位。与以前的报告相反,用我们的抗血清进行免疫染色可检测到肝,大肠,小肠,前列腺和睾丸中的ha丁。我们未在不同年龄患者的可比较组织中发现结核菌素或martin表达的显着发育差异。尽管tuberin和hamartin在大多数组织和细胞类型中共定位,但我们提供的数据表明,在某些组织(包括远端肾单位和内分泌胰腺细胞群)中的细胞中,martin的表达比tuberin丰富。这些数据支持这样的假说,即ha素和结核菌素相互作用并且可能在它们共同表达的许多组织中一起起作用,但是也暗示了ha素在某些细胞类型中具有离散的和专门的功能。

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