Surface distribution of the EGF receptor during differentiation of the human colon carcinoma cell line HT29-D4.

M Lehmann, M Remacle-Bonnet, F Garrouste, J Luis, C Rabenandrasana, J Marvaldi, G Pommier
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引用次数: 6

Abstract

The clone HT29-D4 can be induced to differentiate into enterocyte-like cells, by simply removing glucose from culture medium. In this report, we used the HT29-D4 model to study the membrane segregation of the EGF receptor on epithelial intestinal cells. Differentiated and undifferentiated cells displayed a single class of EGF binding sites with similar dissociation constants. However, differentiation of HT29-D4 led to a 3-fold decrease in the total number of EGF binding sites, while the number of IGF-I binding sites was unchanged. Fifteen percent of EGF receptors present on differentiated HT29-D4 cells were localized in the apical surface, whereas 98% of IGF-I receptors were segregated to the basolateral domain. By covalent cross-linking experiments using 125I-EGF and by immunoprecipitation with an anti-EGF receptor antibody, we have characterized the HT29-D4 EGF receptor as a Mr = 165,000 protein in both differentiated and undifferentiated cells. Apical EGF receptors were functional, as evidenced by their ability to be internalized in response to EGF binding. Thus, intact and functional EGF receptors are present at the apical surface of differentiated HT29-D4 cells, suggesting the presence of EGF receptors on the apical domain of enterocytes.

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人结肠癌细胞系HT29-D4分化过程中EGF受体的表面分布。
通过简单地从培养基中去除葡萄糖,可以诱导克隆HT29-D4分化为肠细胞样细胞。在本报告中,我们采用HT29-D4模型研究了EGF受体在上皮肠细胞上的膜分离。分化细胞和未分化细胞显示出一类具有相似解离常数的EGF结合位点。然而,HT29-D4的分化导致EGF结合位点总数减少3倍,而IGF-I结合位点数量不变。在分化的HT29-D4细胞中,15%的EGF受体位于根尖表面,而98%的IGF-I受体位于基底外侧区域。通过使用125I-EGF的共价交联实验和抗EGF受体抗体的免疫沉淀,我们在分化和未分化细胞中均鉴定出HT29-D4 EGF受体为Mr = 165,000的蛋白。顶端EGF受体是功能性的,因为它们能够内化以响应EGF结合。因此,分化的HT29-D4细胞的根尖表面存在完整的、功能性的EGF受体,提示肠细胞的根尖区域存在EGF受体。
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