索拉非尼联合华蟾素片治疗中晚期原发性肝癌的临床疗效观察被引量：20

Clinical observation of patients with primary liver cancer treated by sorafenib combined cinobufagin tablets

导出

摘要背景与目的:索拉非尼目前已广泛应用于中晚期肝癌的治疗,同时中成药华蟾素在肝癌的辅助治疗中也起到了一定作用。本文观察口服索拉非尼联合华蟾素片治疗中晚期原发性肝癌的临床疗效、不良反应、生活质量及疼痛情况。方法:选择2009年1月—2012年7月经我院确诊为中晚期原发性肝癌的59例患者,随机分成索拉非尼联合华蟾素片治疗组(联合组,n=30)与索拉非尼单药对照组(对照组,n=29)。联合组给予索拉非尼400 mg,每日2次,华蟾素片4片,每日3次;对照组给予单药索拉非尼400 mg,每日2次。4周为1个治疗周期,每两个治疗周期后行MRI等检查评价疗效。结果:临床疗效方面,联合组临床获益率(clinical benefit rate,CBR)明显高于对照组,差异有统计学意义(P<0.05);不良反应方面,联合组腹泻率较对照组高,但差异无统计学意义(P>0.05),未见其他明显增加的不良反应;联合组治疗后白细胞(white blood cell,WBC)、总胆红素(total bilirubin,TBIL)和谷丙转氨酶(alanine aminotransferase,ALT)指标较对照组有明显的改善,差异有统计学意义(P<0.05);在生活质量方面,联合组生活质量改善率明显高于对照组,两组比较差异有统计学意义(P<0.05);在疼痛方面,联合组疼痛缓解率明显高于对照组,差异有统计学意义(P<0.05)。结论:索拉非尼联合华蟾素片是中晚期肝癌一种较理想的治疗选择。 Background and purpose： Sorafenib has been widely used in the treatment of middle-advanced stage liver cancer. At the same time, cinobufagin of traditional Chinese medicines also played an important role in the treatment of liver cancer. Our study was designed to observe the clinical efficacy, adverse effects, quality of life and the pain of patients when sorafenib combined with cinobufagin tablets in the treatment of middle-advanced primary liver cancer. Methods： From Jan. 2009 to Jul. 2012, 59 patients with middle-advanced stage liver cancer were randomly divided into treatment group which treated 30 patients by sorafenib combined with cinobufagin tablets, and control group which treated 29 patients by sorafenib only. Results： The clinical benefit rate （CBR） of the treatment group was better than that of control group, the difference was significant （P〈0.05）. The diarrhea rate of the treatment group was higher than that of control group, but there were no significant differences （P〉0.05）. There was no significant increase in the rate of other adverse effects. The WBC, TBIL, ALT indicator were improved obviously in the control group, the difference was significant P〈0.05）. The life quality of patients in treatment group were improved more significantly than those in control group （P〈0.05）. Cancer pain relief rate in treatment group was significantly higher than that in control group （P〈0.05）. Conclusion： Sorafenib combined with cinobufagin tablets in the treatment of liver cancer, is a good choice for treatment of middle-advanced liver cancer.

作者冯丽华陈毅德郑志高高应勤

机构地区厦门市第二医院肿瘤内科

出处《中国癌症杂志》 CAS CSCD 北大核心 2012年第11期856-859,共4页 China Oncology

关键词索拉非尼华蟾素片原发性肝癌临床疗效 Sorafenib Cinobufagin tablets Primary liver cancer Clinical efficacy

分类号 R735.7 [医药卫生—肿瘤]

引文网络
相关文献

参考文献12

1ALVESI R C, ALVES D, GUZ B, et al. Advanced hepatocellular carcinoma. Review of targeted molecular drugs [ J ] . Ann Hepatol, 2011, 10(1): 21-27.
2PARKIN D M, BRAY F, FERLAY J, et al. Estimating theworld cancer burden: globocan 2000 [ J ] . Int J Cancer, 2001, 94(2): 153-156.
3曹宇华,罗和生.华蟾素治疗晚期肝癌的临床疗效研究[J].中国医学文摘（老年医学）,2007,16(1):18-19. 被引量：5
4杨秉辉,任正刚.原发性肝癌诊断标准[J].中华肝脏病杂志,2000,8(3):135-135. 被引量：626
5THERASSE P, ARBUCK S G, EISENHAUER E A, et al. New guidelines to evaluate the response to treatment in solid tumors [ J ] . J Natl Cancer Inst, 2000, 92(3): 205-216.
6孙燕,石远凯.临床肿瘤内科手册[M].5版.北京:人民卫生出版社,2010:153-156.
7ZHU A X. Development of sorafenib and other molecularly targeted agents in hepatocellular carcinoma [ J ] . Cancer, 2008, 112(2): 250-259.
8LLOVET J M, RICCI S, MAZZAFERRO V, et al. Sharp investigators study group sorafenib in advanced hepatocellular carcinoma [ J ]. N Engl J Med, 2008, 359(7): 378-390.
9CHENG A L, KANG Y K, CHEN Z, et al. Efficacy and safety of sorafenib in patients in the Asia-Pacific region with advanced hepatocellular carcinoma: a phase III randomized, double blind, placebo-controlled trial [ J ] . Lancet Oncol, 2009, 10(1): 25-34.
10陈华,孙宇,崔晓楠.华蟾素注射液对人肝癌HepG-2细胞DNA拓扑异构酶Ⅰ的影响[J].中国癌症杂志,2010,20(3):197-201. 被引量：24

二级参考文献34

1陈建国,宋新明.中国肝癌发病水平的估算及分析[J].中国肿瘤,2005,14(1):28-31. 被引量：93
2朱晓燕（综述）,刘鲁明（审校）.华蟾素注射液及其活性成份抗肿瘤机制的研究进展[J].世界肿瘤杂志,2006,5(4):272-275. 被引量：20
3陈卫华,陈燕,崔国惠.鱼藤素作用K562细胞TopoⅠ表达的探讨[J].中国肿瘤临床,2007,34(3):121-124. 被引量：3
4张莉,李军民,钱樱,王焰,沈志祥.华蟾素诱导U937细胞凋亡及其作用机制[J].肿瘤,2007,27(5):341-344. 被引量：33
5Song IH.Molecular targeting for treatment of advanced hepatocellular carcinoma[J].Korean J Hepatol,2009,15(3):299-308.
6Liu LF.DNA tupoisomerase poisons as antitumor drugs[J].Annu Rev Biochem,1989,58:351-375.
7Giovanella BC,Stehlin JS,Wall ME,et al.DNA topoisomerase Ⅰ-targeted chemotherapy of human colon cancer in xenografts[J].Science,1989,246(4933):1046-1048.
8Potmesil M,Hsiang YH,Liu LF,et al.Resistance of human leukemic and normal lymphocytes to drug-induced DNA cleavage and low levels of DNA topoisomerase Ⅱ[J].Cancer Res,1988,48:3537-3543.
9Rho YH,Lee BW,Park KH,et al.Cudraflavanone A purified from Cudrania tricuspidata induces apoptotic cell death of human leukemia U937 cells,at least in part,through the inhibition of DNA topoisomerase Ⅰ and protein kinase C activity[J].Anti-Cancer Drugs,2007,18(9):1023-1028.
10Sano K,Shuhin T.A study of topoisomerase activity in human tcsticular cancers[J].Anticancer Res,1995,15(5B):2117-2120.