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首页> 外文期刊>Cancer Management and Research >Prognostic and Clinicopathological Significance of EphB3 and Dysadherin Expression in Extrahepatic Cholangiocarcinoma
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Prognostic and Clinicopathological Significance of EphB3 and Dysadherin Expression in Extrahepatic Cholangiocarcinoma

机译:Ephb3和嗜睡素表达在肝胆管癌中的预后和临床病理学意义

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Aim: EphB3 and dysadherin are involved in tumorigenesis and progression of many neoplasms. However, the roles of EphB3 and dysadherin in extrahepatic cholangiocarcinoma (ECC) remain to be revealed. In this study, we aimed to evaluate the expression of EphB3 and dysadherin, and investigate their clinicopathological significance in ECC. Methods: We examined EphB3 and dysadherin expression in 100 ECC, 30 peritumoral tissues, 10 adenoma and 15 normal biliary tract tissues using EnVision immunohistochemistry. The relationship between EphB3 or dysadherin expression and clinicopathological features was evaluated using the χ sup 2/sup test or Fisher’s exact test. The overall survival of ECC patients was analyzed using Kaplan-Meier univariate survival analysis and Log rank tests. Results: We found that EphB3 expression was significantly down-regulated and dysadherin expression was significantly up-regulated in ECC tissues compared with normal tissues ( P 0.01). EphB3 expression was negatively correlated with dysadherin expression in ECC ( P 0.01). The positive rate of EphB3 expression and negative rate of dysadherin expression was significantly higher in patients with well-differentiated type, no lymph node metastasis, no surrounding tissues and organs invasion, early TNM stages (I + II) and radical resection ( P 0.01). The survival of ECC patients with positive EphB3 or negative dysadherin expression was significantly longer than patients with negative EphB3 or positive dysadherin expression ( P 0.01). Cox multivariate analysis demonstrated that negative EphB3 or positive dysadherin expression were independent poor prognostic factors in ECC patients. The ROC curves suggested that EphB3 and dysadherin combined diagnostic efficacy (AUC=0.688, 95%CI: 0.603-0.772) was significantly higher EphB3 diagnostic efficacy?(AUC=0.654, 95%CI: 0.564-0.743) or dysadherin diagnostic efficacy (AUC=0.648, 95%CI: 0.558-0.737) alone. Conclusion: EphB3 and dysadherin are involved in the carcinogenesis and progression of ECC, and ECC patients with negative EphB3 or positive dysadherin expression have a poor prognosis.
机译:目的:EphB3和Dysadherin参与许多肿瘤的肿瘤内酯和进展。然而,EphB3和Dysadherin的作用仍然揭示了肠外胆管癌(ECC)中的含量。在这项研究中,我们旨在评估Ephb3和Dysadherin的表达,并研究了ECC的临床病理学意义。方法:使用设想免疫组织化学检查100ECC,30个腹膜组织,10个腺瘤和15个正常胆道组织中的Ephb3和Dysadherin表达。使用χ 2 测试或Fisher的确切测试评估EphB3或Dysadherin表达和临床病理学特征之间的关系。使用Kaplan-Meier单变量存活分析和日志等级测试分析了ECC患者的整体存活。结果:我们发现,与正常组织相比,EPHB3表达显着下调,心肌表达显着上调ECC组织中(P <0.01)。 EphB3表达与ECC中的Dysadherin表达呈负相关(P <0.01)。患有良好分化的型患者的ephb3表达和消退素表达的负率的阳性率显着高,无淋巴结转移,无周围组织和器官侵袭,早期的TNM阶段(I + II)和激进切除(P <0.01 )。 ECC患者阳性EphB3或阴性残疾蛋白表达的存活率明显高于阴性EphB3或阳性Dysadherin表达的患者(P <0.01)。 Cox多变量分析证明,负ephB3或阳性消化素表达在ECC患者中是独立的预后因子。 ROC曲线表明EphB3和Dysadherin联合诊断疗效(AUC = 0.688,95%CI:0.603-0.772)显着提高了EPHB3诊断疗效?(AUC = 0.654,95%CI:0.564-0.743)或软素诊断疗效(AUC单独= 0.648,95%CI:0.558-0.737)。结论:EphB3和Dysadherin参与ECC的致癌和进展,对阴性EphB3或阳性Dysadherin表达的ECC患者具有较差的预后。

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