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Expression of biomarkers (p53, transforming growth factor alpha, epidermal growth factor receptor, c-erbB-2/neu and the proliferative cell nuclear antigen) in oropharyngeal squamous cell carcinomas

机译:口咽鳞状细胞癌中生物标志物(p53,转化生长因子α,表皮生长因子受体,c-erbB-2 / neu和增殖细胞核抗原)的表达

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摘要

Using immunohistochemistry, expression of p53, transforming growth factor-alpha (TGF-α), epidermal growth factor receptor (EGFR), c-erbB-2/neu and proliferating cell nuclear antigen (PCNA) was examined in 26 fresh frozen tissue specimens of oropharyngeal squamous cell carcinomas (SCCs). p53 gene mutations were examined by polymerase chain reaction (PCR)/DNA sequencing methods in 22 carcinomas. The findings were examined for correlations with patients’ clinicopathological parameters. Expressions of p53 and PCNA were also examined in 21 formalin-fixed corresponding tissues. Of the fresh frozen tissue specimens, 77% (20/26) showed expression and 68% (15/22) showed mutations (substitutions) of the p53, with significant clustering of the mutations in exons 5 (8/22; 36%), 7 (4/22; 18%) and 8 (5/22; 23%). No mutations were found in exon 6. There was a discordance between expression of p53 protein and mutations of the gene. Parallel to expression and mutations of the p53 found in most of the specimens, expression of TGF-α, EGFR, c-erbB-2/neu and PCNA was found in 88% (22/25), 92% (23/25), 58% (14/24) and 91% (21/23) of the specimens, respectively. For the formalin-fixed tissue specimens, 62% (13/21) and 90% (19/21) expressed p53 and PCNA, respectively. Examining for correlations with patients’ clinicopathological parameters, expression of p53, TGF-α, EGFR and c-erbB-2/neu seemed to negatively correlate with the increase of the tumour grade. The present work suggests that: (1) lack of negative growth regulation due to inactivation of the p53 gene together with activation of other proto-oncogenes are necessary genetic events in the carcinogenesis of oropharyngeal SCCs; (2) in oropharyngeal SCCs, p53 gene mutations were clustered in exons 5 (codons 130–186), 7 (codons 230–248) and 8 (codons 271–282) which perhaps suggests that tobacco carcinogens probably affect the mutational hot spots of the p53 gene at codons 157, 175, 186, 248, 273 and 282; and (3) fresh frozen and formalin-fixed tissue specimens give similar results when an immunohistochemical method is applied. The importance of p53, TGF-α, EGFR, c-erbB-2/neu and PCNA as biomarkers in oropharyngeal SCCs deserves particular attention because it might offer further understanding of the development of these carcinomas.
机译:使用免疫组织化学方法,在26例新鲜冰冻组织标本中检测了p53,转化生长因子-α(TGF-α),表皮生长因子受体(EGFR),c-erbB-2 / neu和增殖细胞核抗原(PCNA)的表达。口咽鳞状细胞癌(SCC)。通过聚合酶链反应(PCR)/ DNA测序方法检查了22例癌症中的p53基因突变。检查结果是否与患者的临床病理参数相关。还检测了21个福尔马林固定的相应组织中p53和PCNA的表达。在新鲜的冷冻组织标本中,有77%(20/26)表现出表达,有68%(15/22)表现出p53突变(取代),外显子5中有明显的突变簇(8/22; 36%) ,7(4/22; 18%)和8(5/22; 23%)。在第6外显子中未发现突变。p53蛋白的表达与该基因的突变之间存在不一致。与大多数标本中p53的表达和突变平行,发现TGF-α,EGFR,c-erbB-2 / neu和PCNA的表达分别为88%(22/25),92%(23/25) ,分别为58%(14/24)和91%(21/23)的标本。对于福尔马林固定的组织标本,分别有62%(13/21)和90%(19/21)表达p53和PCNA。检查与患者临床病理参数的相关性,p53,TGF-α,EGFR和c-erbB-2 / neu的表达似乎与肿瘤等级的增加呈负相关。目前的工作表明:(1)由于p53基因失活以及其他原癌基因的激活而导致的负性生长调节缺乏是口咽SCC癌变的必要遗传事件; (2)在口咽SCC中,p53基因突变聚集在第5外显子(130-186密码子),7(第230-248密码子)和8(271-282密码子)中,这可能表明烟草致癌物可能会影响烟草的突变热点。 p53基因在密码子157、175、186、248、273和282处; (3)当采用免疫组织化学方法时,新鲜冷冻和福尔马林固定的组织标本得到相似的结果。 p53,TGF-α,EGFR,c-erbB-2 / neu和PCNA作为口咽SCC中生物标志物的重要性值得特别关注,因为它可能提供对这些癌发展的进一步了解。

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