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Role of E2F-1 and its involving pathway in esophageal squamous cell carcinoma

机译:E2F-1及其参与途径在食管鳞状细胞癌中的作用

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摘要

Background: Esophageal cancer is a lethal disease and the optimal therapy remains unclear. Neoadjuvant chemotherapy provides an increased chance of survival; therefore, we attempted to identify potential molecular markers that might improve evaluations of individual responses to therapy. Methods: We recruited 109 patients with resectable esophageal squamous cell carcinoma. The patients underwent radical esophagectomy and did not receive any other perioperative treatment. Expression of E2F-1 and molecules involved in its targeted pathways, pERK, Bim, pRb, epidermal growth factor receptor, EZH2 and pAKT, was investigated immunohistochemically. Results: Correlations were observed between E2F-1 and pRb expression; EZH2 expression was significantly correlated with the degree of carcinoma differentiation (P = 0.01). Stage III patients were found to have longer survival if they did not express pERK than if they did (23 months vs. 11 months, P = 0.01). Patients with E2F-1 not expressing pRb were found to have longer survival times than those with E2F-1 who expressed pRb (18.8 months vs. 8.6 months, P = 0.021). Similarly, stage III patients with E2F-1 but not expressing pERK also survived longer than those expressing pERK (23.5 months vs. 3.9 months, P 0.001). Conclusions: A high expression of pERK was significantly associated with poor survival in patients with locally advanced esophageal cancer. Expression of a combination of molecules, rather than of individual molecules, was more predictive of disease prognosis. E2F-1 and molecules of its targeted pathways may be candidate proteins as markers of chemosensitivity in esophageal cancer patients.
机译:背景:食道癌是一种致死性疾病,目前尚不清楚最佳治疗方法。新辅助化疗可增加生存机会;因此,我们试图确定潜在的分子标记,这些标记可能会改善对治疗个体反应的评估。方法:我们招募了109例可切除的食管鳞状细胞癌患者。患者接受了根治性食管切除术,未接受任何其他围手术期治疗。免疫组织化学研究了E2F-1及其靶向途径中涉及的分子pERK,Bim,pRb,表皮生长因子受体,EZH2和pAKT的表达。结果:观察到E2F-1与pRb表达之间的相关性。 EZH2表达与癌的分化程度显着相关(P = 0.01)。如果不表达pERK,则III期患者的生存期要比不表达pERK的患者长(23个月对11个月,P = 0.01)。发现不表达pRb的E2F-1患者比表达pRb的E2F-1患者具有更长的生存时间(分别为18.8个月和8.6个月,P = 0.021)。同样,III期E2F-1但不表达pERK的患者也比表达pERK的患者生存更长(23.5个月比3.9个月,P <0.001)。结论:pERK的高表达与局部晚期食管癌患者的不良生存率显着相关。分子组合而不是单个分子的表达更能预测疾病的预后。 E2F-1及其靶向途径的分子可能是候选蛋白,作为食管癌患者化学敏感性的标志。

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