TRA-8抗死亡受体5抗体与CPT-11联合治疗可诱导胰腺癌原位模型中的肿瘤消退。
Combination treatment with TRA-8 anti death receptor 5 antibody and CPT-11 induces tumor regression in an orthotopic model of pancreatic cancer.
作者信息
DeRosier Leo Christopher, Buchsbaum Donald J, Oliver Patsy G, Huang Zhi-Qiang, Sellers Jeffrey C, Grizzle William E, Wang Wenquan, Zhou Tong, Zinn Kurt R, Long Joshua W, Vickers Selwyn M
机构信息
Department of Surgery, University of Alabama at Birmingham, Birmingham, Alabama 35294-6832, USA.
出版信息
Clin Cancer Res. 2007 Sep 15;13(18 Pt 2):5535s-5543s. doi: 10.1158/1078-0432.CCR-07-1075.
PURPOSE
Evaluate the response of human pancreatic cancer cell lines and orthotopic tumors to TRA-8, an agonistic antibody to death receptor 5, in combination with irinotecan (CPT-11).
EXPERIMENTAL DESIGN
MIA PaCa-2 and S2VP10 cells were treated with TRA-8 and/or CPT 11. Cell viability was determined by ATP assay. JC-1 mitochondrial depolarization and Annexin V assays confirmed cell death by apoptosis. Immunoblotting was used to evaluate protein changes. MIA PaCa-2 cells were injected into the pancreas of severe combined immunodeficient mice. Mice underwent abdominal ultrasound to quantitate tumor size before and after treatment with twice weekly injections of 200 microg TRA-8 and/or 25 mg/kg CPT-11 for one or two treatment cycles, each lasting 2 weeks.
RESULTS
MIA PaCa-2 cells were more sensitive to TRA-8 and showed additive cytotoxicity, whereas S2VP10 cells showed synergistic cytotoxicity when treated with TRA-8 and CPT-11. Cell death occurred via apoptosis with increased cleavage of caspase-3, caspase-8, and caspase-9 and proapoptotic proteins Bid and poly(ADP)ribose polymerase after combination treatment compared with either agent alone. XIAP and Bcl-XL inhibitors of apoptosis were down-regulated. After a single cycle of in vivo combination therapy, tumor sizes had diminished significantly (P<0.001) at 8 days posttreatment compared with no treatment, CPT-11, and TRA-8; and there was a 50-day increase in survival with combination treatment over untreated controls (P=0.0002), 30 days over TRA-8, and a 36-day increase over CPT-11 monotherapy (P=0.0003). With two cycles of TRA-8/CPT-11 treatment, mean survival time increased significantly (P<0.001) to 169 days versus untreated controls, TRA-8 or CPT-11 (76, 121, or 108 days, respectively).
CONCLUSIONS
Combination TRA-8 and CPT-11 therapy produced enhanced cytotoxicity and survival in the MIA PaCa-2 orthotopic model of pancreatic cancer.
目的
评估人胰腺癌细胞系和原位肿瘤对TR - 8(一种死亡受体5激动性抗体)联合伊立替康(CPT - 11)的反应。
实验设计
用TR - 8和/或CPT - 11处理MIA PaCa - 2和S2VP10细胞。通过ATP检测确定细胞活力。JC - 1线粒体去极化和膜联蛋白V检测证实细胞凋亡导致的细胞死亡。免疫印迹法用于评估蛋白质变化。将MIA PaCa - 2细胞注射到重度联合免疫缺陷小鼠的胰腺中。小鼠接受腹部超声检查以定量肿瘤大小,在每周两次注射200μg TRA - 8和/或25mg/kg CPT - 11进行一或两个治疗周期(每个周期持续2周)前后进行测量。
结果
MIA PaCa - 2细胞对TR - 8更敏感,显示出相加的细胞毒性,而S2VP10细胞在接受TR - 8和CPT - 11处理时显示出协同细胞毒性。联合治疗后,与单独使用任何一种药物相比,细胞通过凋亡死亡,caspase - 3、caspase - 8和caspase - 9以及促凋亡蛋白Bid和聚(ADP)核糖聚合酶的裂解增加。凋亡抑制蛋白XIAP和Bcl - XL下调。在体内联合治疗的单个周期后,与未治疗、CPT - 11和TR - 8相比,治疗后8天肿瘤大小显著减小(P<0.001);联合治疗组的生存期比未治疗对照组延长50天(P = 0.0002),比TR - 8延长30天,比CPT - 11单药治疗延长36天(P = 0.0003)。经过两个周期的TR - 8/CPT - 11治疗,平均生存时间显著增加(P<0.001)至169天,而未治疗对照组、TR - 8或CPT - 11组分别为76天、121天或108天。
结论
在胰腺癌的MIA PaCa - 2原位模型中,TR - 8与CPT - 11联合治疗产生增强的细胞毒性并延长生存期。
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