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UCP2 expression may represent a predictive marker of neoadjuvant chemotherapy effectiveness for locally advanced uterine cervical cancer

机译:UCP2表达可以代表局部晚期子宫宫颈癌的新辅助化疗效果的预测标志物

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Concurrent chemoradiotherapy is the standard treatment for locally advanced uterine cervical cancer. However, effective neoadjuvant chemotherapy (NAC) can reduce tumor size and facilitate hysterectomy for locally advanced uterine cervical cancer. NAC treatment could improve the prognosis of patients with locally advanced cervical cancer. However, if NAC is ineffective, radiotherapy must be pursued. This causes a delay in initiating the core treatment and results in a worse prognosis. Therefore, the identification of predictive markers of whether NAC is likely to be effective for the treatment of locally advanced uterine cervical cancer could improve patient prognosis. Uncoupling protein 2 (UCP2) is broadly expressed in cancer cells, and suppresses mitochondrial reactive oxygen species (ROS) production. UCP2 contributes to both carcinogenesis and chemoresistance by reducing ROS. Downregulation of UCP2 results in significantly increased cell death following chemotherapy. The present study investigated the association between UCP2 expression and NAC effectiveness. A total of 58 patients with locally advanced uterine cervical cancer (stage IIIA or IIIB) treated at Osaka City University Hospital between April 1995 and March 2010 were examined. Tumor tissue samples were obtained by punch biopsy prior to NAC. UCP2 expression was examined immunohistochemically and scored using a weighted scoring system. Patients were divided into NAC effective (n=34) and ineffective (n=24) groups. Furthermore, UCP2 expression in human uterine cervical cancer cells was inhibited by genipin, and changes in cisplatin sensitivity were examined. UCP2 weighted score was higher in the NAC ineffective group than in the NAC effective group (P=0.038). Additionally, the low UCP2 expression group was more sensitive to NAC than the high UCP2 expression group (P=0.041). Sensitivity to cisplatin was significantly increased when UCP2 was inhibited in human uterine cervical cancer cells in vitro. UCP2 expression may become a predictive marker of whether NAC is effective for patients with locally advanced uterine cervical cancer, which could improve patient prognosis.
机译:同期化疗是局部晚期子宫宫颈癌的标准治疗方法。然而,有效的Neoadjuvant化疗(NAC)可以降低肿瘤大小,促进局部晚期子宫宫颈癌的子宫切除术。 NAC治疗可以改善局部晚期宫颈癌患者的预后。但是,如果NAC是无效的,则必须追踪放射疗法。这导致延迟启动核心处理并导致更差的预后。因此,鉴定NAC的预测标志物可能有效治疗局部晚期子宫宫颈癌可以改善患者预后。非偶像蛋白2(UCP2)在癌细胞中广泛表达,并抑制线粒体反应性氧(ROS)产生。通过减少ROS,UCP2有助于致癌和化学性。 UCP2的下调导致化疗后细胞死亡显着增加。本研究研究了UCP2表达与NAC效能之间的关联。在1995年间于1995年4月至2010年4月在大阪市大学医院治疗了58例局部晚期子宫颈癌(IIIA阶段或IIIB)患者。在NAC之前通过冲头活检获得肿瘤组织样品。 UCP2表达被检查免疫组织化学并使用加权评分系统进行评分。患者分为NAC有效(n = 34),无效(n = 24)组。此外,通过Genipin抑制人子宫子宫颈细胞中的UCP2表达,检查了顺铂敏感性的变化。 NAC无效群体中的UCP2加权分数高于NAC有效基团(P = 0.038)。另外,低UCP2表达组比高UCP2表达组更敏感(P = 0.041)。当UCP2在体外抑制人子宫子宫颈癌细胞时,对顺铂的敏感性显着增加。 UCP2表达可能成为NAC对局部晚期子宫宫颈癌患者有效的预测标记,这可以改善患者预后。

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