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Prognostic significance of p53 protein and X-ray repair cross-complementing protein 1 in non-small cell lung cancer.

机译:p53蛋白和X射线修复交叉互补蛋白1在非小细胞肺癌中的预后意义。

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摘要

OBJECTIVES: p53 and XRCC1 protein expression were evaluated in 54 samples of nonsmall cell lung cancer. PATIENTS AND METHODS: The immunohistochemical method was used for detection of the monitored proteins. Tissue samples were divided according to histopathological tumor type. The results were then compared with basic clinical and histopathological parameters (histopathological type, nuclear grade and TNM tumor stage IA, IB). RESULTS: Statistically significant correlations were found between histopathological type and p53 expression, since P < 0.05 (P = 0.015). Comparing p53 expression with grade resulted in a strong positive correlation (P < 0.0396, R2 = 0.9223). The percentage of p53-positive tumors progressively increased from 0% in grade 1 to 75% in grade 4. No correlation was found between p53 expression and tumor stage. In case of XRCC1, the highest level was found in squamous cell lung carcinoma, where 71% of samples was positive. In case of large cell carcinoma samples, it was 67%, and in adenocarcinoma 52% of samples showed XRCC1 immunoreactivity. No statistically significant correlation was found between histopathological type, grade or early stage (IA, IB) of non-small cell lung cancer and expression of XRCC1 protein profile without neoadjuvant therapy. CONCLUSIONS: We found a statistically significant correlation between p53 expression and histopathological tumor type. It is possible that stabilized p53 protein plays an important role in the development of squamous and large cell carcinoma. Our findings also suggest that p53 expression cumulates with the dedifferentiation of cancer cells. It is possible that the expression of XRCC1 is not fixed and could be changed by the status of cancer cells and in relation to therapy. Relevant data about pre- versus post-chemotherapy and XRCC1 expression are needed to evaluate the influence of XRCC1 on drug resistance.
机译:目的:在54个非小细胞肺癌样本中评估p53和XRCC1蛋白的表达。患者与方法:采用免疫组织化学方法检测被监测蛋白。根据组织病理学肿瘤类型对组织样品进行划分。然后将结果与基本临床和组织病理学参数(组织病理学类型,核分级和TNM IA,IB期肿瘤)进行比较。结果:由于P <0.05(P = 0.015),因此在组织病理学类型与p53表达之间存在统计学上的显着相关性。将p53表达与等级进行比较可得出很强的正相关性(P <0.0396,R2 = 0.9223)。 p53阳性肿瘤的百分比从1级的0%逐渐增加到4级的75%。p53表达与肿瘤分期之间没有相关性。对于XRCC1,在鳞状细胞肺癌中发现最高水平,其中71%的样本呈阳性。在大细胞癌样本中,这一比例为67%,在腺癌中,有52%的样本显示出XRCC1免疫反应性。非小细胞肺癌的组织病理学类型,分级或早期(IA,IB)与未经新辅助治疗的XRCC1蛋白谱表达之间无统计学意义的相关性。结论:我们发现p53表达与组织病理学肿瘤类型之间具有统计学意义的相关性。稳定的p53蛋白可能在鳞状和大细胞癌的发展中起重要作用。我们的发现还表明,p53表达随着癌细胞的去分化而累积。 XRCC1的表达可能不固定,可能会因癌细胞的状态以及与治疗的关系而改变。需要有关化疗前后,XRCC1表达的相关数据,以评估XRCC1对耐药性的影响。

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