Kim Hong-Beum, Cho Won Jin, Choi Nam Gyu, Kim Sung-Soo, Park Jun Hee, Lee Hee-Jeong, Park Sang Gon
Department of Premedical Course, Chosun University School of Medicine, Gwangju, Korea.
Department of Urology, Chosun University Hospital, Gwangju, Korea.
Ann Surg Treat Res. 2017 Jan;92(1):15-22. doi: 10.4174/astr.2017.92.1.15. Epub 2016 Dec 30.
Biliary cancer is a highly malignant neoplasm with poor prognosis and most patients need to undergo palliative chemotherapy, however major clinical problem associated with the use of chemotherapy is chemoresistance. So far, we aimed at investigating clinical implications of apurinic/apyrimidinic endodeoxyribonuclease 1 (APEX1) and Jagged1 as chemoresistance factors in biliary tract cancer.
We used 5 human biliary tract cancer cell lines (SNU-245, SNU-308, SNU-478, SNU-1079, and SNU-1196), and investigated the chemosensitivity of APEX1 and Jagged1 through 3-(4, 5-dimethylthiazol-2-yl)-2, 5-diphenyltetrazolium bromide (MTT) assay and Western blot. Alternately, the 10 patients of advanced biliary cancer consist of 2 group according to the chemotherapy response examined by immunohistochemistry using APEX1 and Jagged1 antibody, and protein expression level was scored for staining intensity and percent positive cell.
The result of MTT assay after APEX1 knockdown showed that strong coexpression of APEX1 and Jagged1 cell line (SNU-245, SNU-1079, and SNU-1196) showed a greater decrease in IC of chemotherapeutic agent (5-fluorouracil, gemcitabine and cisplatin). The Western blot analysis of APEX1 and Jagged1 expression in biliary cancer cell lines after APEX1 knockdown definitively demonstrated decreased Jagged1 expression. The APEX1 and Jagged1expression level of immunohistochemistry represented that chemorefractory patients had higher than chemoresponsive patients.
These results demonstrate that simultaneous high expression of APEX1 and Jagged1 is associated with chemoresistance in biliary cancer and suggest that is a potential therapeutic target for chemoresistance in advanced biliary cancer.
胆管癌是一种预后较差的高恶性肿瘤,大多数患者需要接受姑息化疗,然而与化疗使用相关的主要临床问题是化疗耐药性。到目前为止,我们旨在研究脱嘌呤/脱嘧啶内切脱氧核糖核酸酶1(APEX1)和锯齿蛋白1作为胆管癌化疗耐药因素的临床意义。
我们使用了5种人胆管癌细胞系(SNU - 245、SNU - 308、SNU - 478、SNU - 1079和SNU - 1196),并通过3 -(4,5 - 二甲基噻唑 - 2 - 基)- 2,5 - 二苯基四氮唑溴盐(MTT)法和蛋白质印迹法研究APEX1和锯齿蛋白1的化学敏感性。另外,10例晚期胆管癌患者根据使用APEX1和锯齿蛋白1抗体通过免疫组织化学检查的化疗反应分为2组,并对蛋白质表达水平的染色强度和阳性细胞百分比进行评分。
APEX1敲低后的MTT试验结果表明,APEX1和锯齿蛋白1强共表达的细胞系(SNU - 245、SNU - 1079和SNU - 1196)化疗药物(5 - 氟尿嘧啶、吉西他滨和顺铂)的IC下降幅度更大。APEX1敲低后胆管癌细胞系中APEX1和锯齿蛋白1表达的蛋白质印迹分析明确显示锯齿蛋白1表达降低。免疫组织化学的APEX1和锯齿蛋白1表达水平表明,化疗难治性患者高于化疗反应性患者。
这些结果表明,APEX1和锯齿蛋白1的同时高表达与胆管癌的化疗耐药性相关,并表明其是晚期胆管癌化疗耐药的潜在治疗靶点。
