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表皮生长因子(EGF)受体、EGF样因子及c-myc在卵巢癌和宫颈癌中的表达及其潜在临床意义。

The expression of EGF receptors, EGF-like factors and c-myc in ovarian and cervical carcinomas and their potential clinical significance.

作者信息

Kohler M, Janz I, Wintzer H O, Wagner E, Bauknecht T

机构信息

Institut für Biologie, Universität Freiburg, F.R.G.

出版信息

Anticancer Res. 1989 Nov-Dec;9(6):1537-47.

PMID:2697181
Abstract

The expression of the epidermal growth factor receptor (EGF-R) and the c-myc oncogene was investigated in different specimens of ovarian and cervical carcinomas. The EGF-Rs were analyzed by EGF binding assay, immunohistochemistry and Northern blotting. For analysis of c-myc expression, we used Northern blotting and immunohistochemistry. Furthermore, tissue concentrations of EGF-like factors (EGF-F) were measured in the same tumor and non-malignant specimens. The biochemical determination of EGF-R demonstrated that EGF specific binding sites were detected in 36% of ovarian (n = 140) and 81% of cervical carcinomas (n = 42). High amounts of EGF-R (greater than 10 fmol/mg specific binding) were found in 8% of the ovarian and 41% of the cervical carcinomas. Increased expression of EGF-R specific mRNA was detectable in 7/21 ovarian and in 5/7 cervical carcinomas. A positive correlation between the amounts of EGF-R mRNA, the EGF-R binding data and the staining index of EGF-R immunohistochemistry was found. The EGF-R immunohistochemistry demonstrates that only the tumor cells produce increased amounts of EGF-R, while the stromal cells are EGF-R negative. Low amounts of EGF-R specific mRNA were also detected in biochemically EGF-R negative tumors. The c-myc specific mRNA signal was found in all cases investigated. It is shown that the c-myc expression was increased in 10/21 ovarian and 5/7 cervical carcinomas. There was no positive correlation between the amounts of EGF-R and c-myc mRNAs. The product of myc, as detected by immunohistochemistry, is found in tumor as well as in stromal cells. The levels of EGF-F were measured in extracts of 63 ovarian and 12 cervical carcinomas and in 21 non-malignant tissues. About 30% of the tumor extracts contained higher EGF-F levels (4-15 ng/mg) than those found in the non-malignant specimens. Tumors with high EGF-F levels expressed high amounts of c-myc RNA. The EGF-R status (n = 111) and the EGF-F levels (n = 63) were related to the prognosis of survival for patients with ovarian carcinomas. EGF-R positive (EGF-R(+)) ovarian carcinomas had a significantly higher response rate to chemotherapy. The survival time of the EGF-R(+) group is reduced compared to the EGF-R negative (EGF-R(-)) group if only patients in remission are used to construct survival curves. Furthermore, a poor prognosis for survival was noticed for ovarian carcinoma patients with high EGF-F levels.

摘要

对不同的卵巢癌和宫颈癌标本中表皮生长因子受体(EGF-R)和c-myc癌基因的表达进行了研究。通过EGF结合试验、免疫组织化学和Northern印迹法分析EGF-R。对于c-myc表达的分析,我们采用了Northern印迹法和免疫组织化学。此外,还在相同的肿瘤和非恶性标本中测量了EGF样因子(EGF-F)的组织浓度。EGF-R的生化测定表明,在36%的卵巢癌(n = 140)和81%的宫颈癌(n = 42)中检测到EGF特异性结合位点。在8%的卵巢癌和41%的宫颈癌中发现了大量的EGF-R(大于10 fmol/mg特异性结合)。在7/21的卵巢癌和5/7的宫颈癌中可检测到EGF-R特异性mRNA表达增加。发现EGF-R mRNA量、EGF-R结合数据与EGF-R免疫组织化学染色指数之间呈正相关。EGF-R免疫组织化学表明,只有肿瘤细胞产生增加量的EGF-R,而基质细胞为EGF-R阴性。在生化检测为EGF-R阴性的肿瘤中也检测到少量的EGF-R特异性mRNA。在所有研究病例中均发现了c-myc特异性mRNA信号。结果表明,在10/21的卵巢癌和5/7的宫颈癌中c-myc表达增加。EGF-R和c-myc mRNA量之间没有正相关。通过免疫组织化学检测到的myc产物在肿瘤细胞和基质细胞中均有发现。在63例卵巢癌、12例宫颈癌和21例非恶性组织的提取物中测量了EGF-F水平。约30%的肿瘤提取物中EGF-F水平(4 - 15 ng/mg)高于非恶性标本。EGF-F水平高的肿瘤表达大量的c-myc RNA。EGF-R状态(n = 111)和EGF-F水平(n = 63)与卵巢癌患者的生存预后相关。EGF-R阳性(EGF-R(+))的卵巢癌对化疗的反应率显著更高。如果仅使用缓解期患者构建生存曲线,EGF-R(+)组的生存时间比EGF-R阴性(EGF-R(-))组缩短。此外,EGF-F水平高的卵巢癌患者生存预后较差。

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