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表达人角蛋白8的转基因小鼠的胰腺外分泌疾病

Exocrine pancreatic disorders in transsgenic mice expressing human keratin 8.

作者信息

Casanova M L, Bravo A, Ramírez A, Morreale de Escobar G, Were F, Merlino G, Vidal M, Jorcano J L

机构信息

Cell and Molecular Biology, Centro de Investigaciones Energéticas, Medioambíentales y Technológicas, E-28040 Madrid, Spain.

出版信息

J Clin Invest. 1999 Jun;103(11):1587-95. doi: 10.1172/JCI5343.

Abstract

Keratins K8 and K18 are the major components of the intermediate-filament cytoskeleton of simple epithelia. Increased levels of these keratins have been correlated with various tumor cell characteristics, including progression to malignancy, invasive behavior, and drug sensitivity, although a role for K8/K18 in tumorigenesis has not yet been demonstrated. To examine the function of these keratins, we generated mice expressing the human K8 (hk8) gene, which leads to a moderate keratin-content increase in their simple epithelia. These mice displayed progressive exocrine pancreas alterations, including dysplasia and loss of acinar architecture, redifferentiation of acinar to ductal cells, inflammation, fibrosis, and substitution of exocrine by adipose tissue, as well as increased cell proliferation and apoptosis. Histological changes were not observed in other simple epithelia, such as the liver. Electron microscopy showed that transgenic acinar cells have keratins organized in abundant filament bundles dispersed throughout the cytoplasm, in contrast to control acinar cells, which have scarce and apically concentrated filaments. The phenotype found was very similar to that reported for transgenic mice expressing a dominant-negative mutant TGF-beta type II receptor (TGFbetaRII mice). We show that these TGFbetaRII mutant mice also have elevated K8/K18 levels. These results indicate that simple epithelial keratins play a relevant role in the regulation of exocrine pancreas homeostasis and support the idea that disruption of mechanisms that normally regulate keratin expression in vivo could be related to inflammatory and neoplastic pancreatic disorders.

摘要

角蛋白K8和K18是单层上皮细胞中间丝细胞骨架的主要成分。这些角蛋白水平的升高与多种肿瘤细胞特征相关,包括向恶性进展、侵袭行为和药物敏感性,尽管K8/K18在肿瘤发生中的作用尚未得到证实。为了研究这些角蛋白的功能,我们培育了表达人K8(hk8)基因的小鼠,这导致它们的单层上皮细胞中角蛋白含量适度增加。这些小鼠表现出进行性外分泌胰腺改变,包括发育异常和腺泡结构丧失、腺泡细胞向导管细胞的再分化、炎症、纤维化以及外分泌组织被脂肪组织替代,同时细胞增殖和凋亡增加。在其他单层上皮组织如肝脏中未观察到组织学变化。电子显微镜显示,与对照腺泡细胞相比,转基因腺泡细胞中的角蛋白以丰富的丝束形式组织,分散在整个细胞质中,而对照腺泡细胞中的丝束稀少且集中在顶端。发现的表型与表达显性负性突变型TGF-β II型受体的转基因小鼠(TGFβRII小鼠)报道的表型非常相似。我们发现这些TGFβRII突变小鼠的K8/K18水平也升高。这些结果表明,单层上皮角蛋白在调节外分泌胰腺稳态中起相关作用,并支持这样一种观点,即体内正常调节角蛋白表达的机制的破坏可能与胰腺炎症和肿瘤性疾病有关。

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