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Enhanced expression of epidermal growth factor receptor correlates with alterations of chromosome 7 in human pancreatic cancer.

机译:表皮生长因子受体的表达增强与人类胰腺癌中7号染色体的改变有关。

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摘要

Recently, the gene for the epidermal growth factor (EGF) receptor has been mapped to chromosome 7p, the short arm of chromosome 7 [Shimizu, N., Kondo, I., Gamou, M. A., Behzadian, A. & Shimizu, Y. (1984) Somatic Cell Mol. Genet. 10, 45-53]. Utilizing EGF binding in saturation studies, karyology, and cDNA hybridization experiments, we have sought to determine whether there is a correlation between dosage or alteration of chromosome 7 and enhanced expression of EGF receptor in cultured human pancreatic carcinoma cells. Saturation binding studies with 125I-labeled EGF were performed at 4 degrees C with four established human pancreatic cancer cell lines: T3M4, PANC-1, COLO 357, and UACC-462. Analysis of binding data revealed enhanced numbers of EGF receptors in all four cell lines. Chromosome banding analysis revealed clonal structural alterations of chromosome 7p in the cell lines T3M4, PANC-1, and COLO 357, whereas UACC-462 displayed multiple copies of chromosome 7. Hybridization studies using a radiolabeled EGF receptor cDNA probe failed to demonstrate DNA sequence amplification in any cell line but confirmed the presence of EGF receptor mRNA in these cells in approximate proportion to EGF receptor number. Our results suggest that enhanced expression of EGF receptor in human pancreatic cancer can be associated with either structural or numerical alterations of chromosome 7.
机译:最近,表皮生长因子(EGF)受体的基因已定位到7p染色体,即7号染色体的短臂[Shimizu,N.,Kondo,I.,Gamou,MA,Behzadian,A.&Shimizu,Y.。 (1984)Somatic Cell Mol。基因10,45-53]。利用EGF结合在饱和度研究,核电学和cDNA杂交实验中,我们试图确定在培养的人胰腺癌细胞中7号染色体的剂量或改变与EGF受体表达增强之间是否存在相关性。用125 I标记的EGF在4℃下用四种已建立的人胰腺癌细胞系:T3M4,PANC-1,COLO 357和UACC-462进行饱和结合研究。结合数据的分析显示,在所有四个细胞系中EGF受体的数量均增加。染色体条带分析显示,T3M4,PANC-1和COLO 357细胞系中7p染色体的克隆结构发生了变化,而UACC-462显示了7号染色体的多个副本。使用放射性标记的EGF受体cDNA探针进行的杂交研究未能证明DNA序列扩增在任何细胞系中,但证实这些细胞中EGF受体mRNA的存在与EGF受体数量大致成比例。我们的结果表明,人类胰腺癌中EGF受体的表达增强可能与7号染色体的结构或数字改变有关。

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