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非洲爪蟾XTC细胞的钙黏蛋白转染会下调底物黏附分子的表达。

Cadherin transfection of Xenopus XTC cells downregulates expression of substrate adhesion molecules.

作者信息

Finnemann S, Kühl M, Otto G, Wedlich D

机构信息

Abteilung Biochemie, Universität Ulm, Germany.

出版信息

Mol Cell Biol. 1995 Sep;15(9):5082-91. doi: 10.1128/MCB.15.9.5082.

Abstract

Cadherins are discussed not in terms of their adhesive function but rather as morphoregulatory proteins. Changes in gene expression following cadherin transfection of cells in culture or by overexpression in embryos have, until now, not been reported. We established a protocol for stable transfection of Xenopus XTC cells and generated cells bearing high levels of membrane-integrated mouse uvomorulin (E-cadherin) or Xenopus XB-cadherin. These cell lines showed drastically impaired substrate adhesion on fibronectin and laminin. In immunoblot and radioimmunoprecipitation experiments, we found that fibronectin and alpha 3/beta 1 integrin are downregulated. The reduced amounts of proteins result from a decrease of the respective mRNAs as proven by RNase protection assays. Coprecipitations revealed that transfected cadherin molecules are complexed with alpha-catenin and beta-catenin at plasma membranes. However, the alpha-catenin present in the XB-cadherin complex differs immunologically from that found in the uvomorulin complex. When a truncated form of XB-cadherin lacking 38 of the most C-terminal amino acids was expressed in XTC cells, complex formation with endogenous catenins was abolished. In these transfectants, substrate adhesion was not affected. These results prove that complex formation of transfected cadherins in XTC cells with endogenous beta-catenin correlates with altered synthesis of certain substrate adhesion molecules.

摘要

钙黏着蛋白并非因其黏附功能而被讨论,而是作为形态调节蛋白。迄今为止,尚未报道过在培养细胞中进行钙黏着蛋白转染或在胚胎中过表达后基因表达的变化。我们建立了非洲爪蟾XTC细胞稳定转染的方案,并生成了高水平膜整合小鼠尿膜素(E-钙黏着蛋白)或非洲爪蟾XB-钙黏着蛋白的细胞。这些细胞系在纤连蛋白和层粘连蛋白上的底物黏附能力大幅受损。在免疫印迹和放射免疫沉淀实验中,我们发现纤连蛋白和α3/β1整合素被下调。如核糖核酸酶保护试验所证实,蛋白质数量的减少是由于各自信使核糖核酸的减少。共沉淀显示,转染的钙黏着蛋白分子在质膜上与α-连环蛋白和β-连环蛋白形成复合物。然而,XB-钙黏着蛋白复合物中的α-连环蛋白在免疫学上与尿膜素复合物中的α-连环蛋白不同。当在XTC细胞中表达一种缺失最末端38个氨基酸的截短形式的XB-钙黏着蛋白时,与内源性连环蛋白的复合物形成被消除。在这些转染细胞中,底物黏附不受影响。这些结果证明,XTC细胞中转染的钙黏着蛋白与内源性β-连环蛋白的复合物形成与某些底物黏附分子合成的改变相关。

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