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转基因小鼠胰岛细胞中表皮细胞角蛋白的异位合成会干扰细胞骨架秩序和胰岛素生成。

Ectopic synthesis of epidermal cytokeratins in pancreatic islet cells of transgenic mice interferes with cytoskeletal order and insulin production.

作者信息

Blessing M, Rüther U, Franke W W

机构信息

Division of Cell Biology, German Cancer Research Center, Heidelberg, Federal Republic of Germany.

出版信息

J Cell Biol. 1993 Feb;120(3):743-55. doi: 10.1083/jcb.120.3.743.

Abstract

The members of the multigene family of intermediate filament (IF) proteins are expressed in various combinations and amounts that are specific for a given pathway or state of differentiation. Previous experiments in which the cell type-specific IF cytoskeleton was altered by introducing foreign IF proteins into cultured cells or certain tissues of transgenic animals have shown a remarkable tolerance, without detectable interference with cell functions. To examine the importance of the cell type-specific cytokeratin (CK) IF pattern, we have studied the ectopic expression of CK genes in different epithelia of transgenic mice. Here we report changes observed in the beta cells of pancreatic islets expressing the genes for human epidermal CKs 1 and/or 10 brought under control of the rat insulin promoter. Both genes were efficiently expressed, resulting in the appearance of numerous and massive bundles of aggregated IFs, resembling those of epidermal keratinocytes. While the synthesis of epidermal CK 10 was readily accommodated and compatible with cell function, mice expressing CK 1 in their beta cells, alone or in combination with CK 10, developed a special form of diabetes characterized by a drastic reduction of insulin-secretory vesicles and of insulin-and CK 1-producing cells. In many CK 1-producing cells, accumulations of fibrous or granular material containing CK 1 were also seen in the nucleus. This demonstration of functional importance of the specific CK-complement in an epithelial cell indicates a contribution of cell type-specific factors to cytoplasmic IF compartmentalization and that the specific CK complement can be crucial for functions and longevity of a given kind of epithelium.

摘要

中间丝(IF)蛋白多基因家族的成员以特定于给定分化途径或状态的各种组合和数量表达。先前的实验通过将外源IF蛋白引入培养细胞或转基因动物的某些组织来改变细胞类型特异性IF细胞骨架,结果显示出显著的耐受性,且未检测到对细胞功能的干扰。为了研究细胞类型特异性细胞角蛋白(CK)IF模式的重要性,我们研究了转基因小鼠不同上皮细胞中CK基因的异位表达。在此,我们报告了在大鼠胰岛素启动子控制下表达人表皮CKs 1和/或10基因的胰岛β细胞中观察到的变化。这两个基因均有效表达,导致出现大量聚集的IF束,类似于表皮角质形成细胞的IF束。虽然表皮CK 10的合成易于适应且与细胞功能相容,但在β细胞中单独或与CK 10联合表达CK 1的小鼠,发展出一种特殊形式的糖尿病,其特征是胰岛素分泌囊泡以及产生胰岛素和CK 1的细胞急剧减少。在许多产生CK 1的细胞中,细胞核中也可见到含有CK 1的纤维状或颗粒状物质的积累。上皮细胞中特定CK互补物功能重要性的这一证明表明细胞类型特异性因子对细胞质IF区室化有贡献,并且特定的CK互补物对于给定类型上皮细胞的功能和寿命可能至关重要。

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