肺抑瘤合剂治疗肺癌及其对抑癌基因P53调控作用的临床与实验研究
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摘要
本研究的目的是通过临床与实验研究观察肺抑瘤合剂治疗中晚期肺癌的疗
效并探讨其作用机理。方法:将78例经细胞学、病理学确诊的原发性支气管肺
癌患者随机分为以本药和化疗的联合治疗组(简称治疗组,39例)与单纯化疗
组(简称对照组,39例)进行临床疗效观察;实验研究观察本药对p53抑癌基
因的调控作用。结果:临床结果表明治疗组在改善症状、提高生活质量、稳定病
灶、延长生存期、提高化疗临床疗效及减轻化疗毒副作用等方面均优于对照组
(P<0. 05或P<0. 01) 。动物实验表明本药能显著抑制肺癌小鼠局部肿瘤生长及自
发性癌转移;能明显延长荷瘤小鼠生存期;其机理可能在于肺抑瘤合剂对p53抑
癌基因的调控。
Objective: To observe the effects on the treating the lung cancer and the influence of the expression for p53 protein with Fei Yi Liu He Ji. Methods:78 confirmed primary lung cancer patients were randomly divided into two groups . 39 patients of the treated group were treated with Fei Yi Liu He Ji mixture and chemotherapy. 39 patients in control group were treated with chemotherapy, and the clinical therapeutic effects were observed. In the mouse experimental study, we observed the 4 groups' effects of treating the mouse model of lung cancer with Fei Yi Liu He Ji, Fei Yi Liu He Ji plus p53 protein and the p53 protein. Results: The clinical study showed the therapeutic effects of the treated group were more significant than it of the control group(P<0. 05 or P<0. 01).We also found the immune index increased and the toxic reaction caused by the chemotherapy reduced significantly in the treated group. In the experimental study, Fei Yi Liu He Ji and p53 gene can obviously inhibit the growth of tumor .The differe
nce wes significant between the four groups, among which the combined Fei Yi Liu He Ji and p53 gene enhance the inhibiting effect more markedly. The survival period of tumor bearing nude mice was prolonged after transfecting p53 gene or Fei Yi Liu He Ji alone, p53 gene or Fei Yi Liu He Ji jointly can prolong the survival period significantly. Conclusion: Fei Yi Liu He Ji mixture plus chemotherapy has better effects on inhibiting tumor than chemotherapy
does. And Fei Yi Liu He Ji mixture can reduce the toxic reaction caused by the chemotherapy. The functionary mechanism for its restraining cancer may be relative to its restraining the expression for the protein p53.
效并探讨其作用机理。方法:将78例经细胞学、病理学确诊的原发性支气管肺
癌患者随机分为以本药和化疗的联合治疗组(简称治疗组,39例)与单纯化疗
组(简称对照组,39例)进行临床疗效观察;实验研究观察本药对p53抑癌基
因的调控作用。结果:临床结果表明治疗组在改善症状、提高生活质量、稳定病
灶、延长生存期、提高化疗临床疗效及减轻化疗毒副作用等方面均优于对照组
(P<0. 05或P<0. 01) 。动物实验表明本药能显著抑制肺癌小鼠局部肿瘤生长及自
发性癌转移;能明显延长荷瘤小鼠生存期;其机理可能在于肺抑瘤合剂对p53抑
癌基因的调控。
Objective: To observe the effects on the treating the lung cancer and the influence of the expression for p53 protein with Fei Yi Liu He Ji. Methods:78 confirmed primary lung cancer patients were randomly divided into two groups . 39 patients of the treated group were treated with Fei Yi Liu He Ji mixture and chemotherapy. 39 patients in control group were treated with chemotherapy, and the clinical therapeutic effects were observed. In the mouse experimental study, we observed the 4 groups' effects of treating the mouse model of lung cancer with Fei Yi Liu He Ji, Fei Yi Liu He Ji plus p53 protein and the p53 protein. Results: The clinical study showed the therapeutic effects of the treated group were more significant than it of the control group(P<0. 05 or P<0. 01).We also found the immune index increased and the toxic reaction caused by the chemotherapy reduced significantly in the treated group. In the experimental study, Fei Yi Liu He Ji and p53 gene can obviously inhibit the growth of tumor .The differe
nce wes significant between the four groups, among which the combined Fei Yi Liu He Ji and p53 gene enhance the inhibiting effect more markedly. The survival period of tumor bearing nude mice was prolonged after transfecting p53 gene or Fei Yi Liu He Ji alone, p53 gene or Fei Yi Liu He Ji jointly can prolong the survival period significantly. Conclusion: Fei Yi Liu He Ji mixture plus chemotherapy has better effects on inhibiting tumor than chemotherapy
does. And Fei Yi Liu He Ji mixture can reduce the toxic reaction caused by the chemotherapy. The functionary mechanism for its restraining cancer may be relative to its restraining the expression for the protein p53.
引文
[1] 查人俊.现代肺癌诊断与治疗.北京:人民军区出版社,1993,第一版: 291-294
[2] 查人俊.现代肺癌诊断与治疗.北京:人民军医出版社,1993,264-267
[3] 查人俊 5. 现代肺癌诊断与治疗.北京:人民军医出版社,1993,92-97, 292
[4] 中华人民共和国卫生部药政局.新药(中药)临床研究指导原则(第二 版),1988:24
[5] 查人俊,等.现代肺癌诊断与治疗.北京:人民军区出版社,1993,第一 版:92-93
[6] 沈金鳌.杂病源流犀炷,上海科学技术出版社,1962,第一版:363
[7] 顾松圆.顾松圆医镜,郑州:河南人民出版社,1961,第一版:112
[8] 华佗.中藏经,南京:江苏科学技术出版社,1985,第一版:45
[9] 华佗.中藏经,南京:江苏科学技术出版社,1985,第一版:49
[10] 阴健,等.中药现代研究与临床应用.北京:学苑出版社,第一版, 1993:12. 13. 14. 594. 595. 242
[11] 赵瑾.抗肿瘤补益中药对免疫功能影响的研究近况.中成药研 究.1998,(5) :26
[12] 李美芬,等.黄芪促进小鼠粒系选血.湖南医科大学学 报.1991,16(2) :135
[13] 谢伯玲,等.黄芪注射液对大白鼠造血功能的影响.南京中医学院学 报.1988,(4) :41
[14] 谢伯玲,等.黄芪注射液对大白鼠造血功能的影响.南京中医学院学 报.1989,(1) :43
[15] 吴广,等.参芪注射液配合化疗治疗恶性肿瘤的临床观察.北京中医药 大学学报.1997,20(2) :50-51
[16] 陈良良,等.新加沙参麦冬汤治疗原发性肺癌的临床和实验研究.浙江 中医杂志.1997,(6) :247-248
[17] 韩明权,等.24味中药对人肺腺癌细胞核酸和蛋白质及细胞周期影响
的观察.中国中西医结合杂志.1995,15(3:147-149)
[18] 郭瑞林.扶正祛邪与肿瘤免疫.实用中西医结合杂志.1991,4:205
[19] 李家庚,等.中医肿瘤防治大全.北京:科学技术文献出版社,1994, 第1版:627. 607. 608. 587. 588
[20] 余桂清.恶性肿瘤中医治则治法研究进展,实用中西医结合杂志, 1991,4:205
[21] 唐文秀,等.中医药治疗原发性非小细胞肺癌临床观察中医杂志 1994,35(5) :284
[22] 郁仁存.中国肿瘤学(下册),北京:科学出版社,1985,第1版:147,204
[23] 潘敏求.中华肿瘤治疗大成.石家庄:河北科学技术出版社,1996,第1 版:55
[24] 王浴生.中药药理与应用,北京:人民卫生出版社,1983,第1版:326-330
[25] 雷海鹏,等.关于抗肿瘤药物的研究.药学学报.1063,(4) :199
[26] 赵锡民,等.清癌痛合复元汤治疗癌痛50例.山东中医杂志.1992;(5) : 20
[27] 李维廉,等.扶正女贞素对肿瘤放、化疗后患者免疫功能影响的临床研 究.全国第三届扶正培本防治研究学术研讨会论文汇编.1989:6-9
[28] 廖美琳.等.化疗在肺癌重的应用发展.见秦叔达.王建民,王杰军主 编.中国临床肿瘤学教育专辑(2001) .北京:中国医药科技出版社. 2001,12
[29] 杨宇飞,吴煜,姚晨.非小细胞肺癌中医临床研究方法探讨.见秦叔达, 王建民,王杰军主编.中国临床肿瘤学教育专辑(2001) .北京:中国 医药科技出版社.2001,61
[30] 王金荣,常春运.王知佳.扶正消积法治疗肺癌64例.辽宁中医杂志. 1996,23(1) :495
[31] 张珍玉.灵枢经语释,济南:山东科技出版社,1983,第1版:51
[32] 南京中医学院医学教研组.皇帝内经素问诊释,上海:上海科技出版社, 1961,第1版:122
[33] 周风梧,等.皇帝内经素问白话解,北京:人民卫生出版社,1958,第1 版:254
[34] 赵佶.圣济总录(上册),北京:人民卫生出版社,1962,第1版:1274
[35] 陈实功.外科正宗,上海:上海科学技术出版社,1989,第1版:326
[36] 张景岳.景岳全书,北京:人民卫生出版社,1991,第1版:354
[37] 魏鸿.医学实验动物学.成都:四川科技出版社,1998,423-427
[38] 姜泊,张亚历,周殿元.分子生物学常用实验方法.北京:人民军医出 版社,1996,103-162
[39] Harlow E, Williamson NM, Ralston R ,et al. Molecular cloning and in vitro expression of a cDNA clone for human cellnlar tumor antigen p53. Mol Cell Biol, 1985,5:1601-1610
[40] Serrano M, Hannon GL, Beach D. A new regulatory motif in cell-cycle control causing specific inhibition of cyclin D/CDK4. Nature, 1993,366:704-707
[41] 杨静平,孔玉英,林其谁.SA脂质体-高效介导DNA转染的新试剂.生 物化学与生物物理学报,1993,25:231-273
[42] 姜泊.细胞凋亡基础与临床.北京:人民军医出版社,1999,53
[43] 孙靖中,皱雄.肿瘤分子生物学.北京:人民卫生出版社,1998,119
[44] LaneDp. ADeathintheLifeofp53. Nature,1993;362(6423) : 7864
[45] LaneDp. p53,guardianoftheGenome.Nature,1992:358(6381) : 15-165
[46] 刘鸿君.p53基因突变与致癌作用.国外医学卫生学分 册,1996:23(2) :39
[2] 查人俊.现代肺癌诊断与治疗.北京:人民军医出版社,1993,264-267
[3] 查人俊 5. 现代肺癌诊断与治疗.北京:人民军医出版社,1993,92-97, 292
[4] 中华人民共和国卫生部药政局.新药(中药)临床研究指导原则(第二 版),1988:24
[5] 查人俊,等.现代肺癌诊断与治疗.北京:人民军区出版社,1993,第一 版:92-93
[6] 沈金鳌.杂病源流犀炷,上海科学技术出版社,1962,第一版:363
[7] 顾松圆.顾松圆医镜,郑州:河南人民出版社,1961,第一版:112
[8] 华佗.中藏经,南京:江苏科学技术出版社,1985,第一版:45
[9] 华佗.中藏经,南京:江苏科学技术出版社,1985,第一版:49
[10] 阴健,等.中药现代研究与临床应用.北京:学苑出版社,第一版, 1993:12. 13. 14. 594. 595. 242
[11] 赵瑾.抗肿瘤补益中药对免疫功能影响的研究近况.中成药研 究.1998,(5) :26
[12] 李美芬,等.黄芪促进小鼠粒系选血.湖南医科大学学 报.1991,16(2) :135
[13] 谢伯玲,等.黄芪注射液对大白鼠造血功能的影响.南京中医学院学 报.1988,(4) :41
[14] 谢伯玲,等.黄芪注射液对大白鼠造血功能的影响.南京中医学院学 报.1989,(1) :43
[15] 吴广,等.参芪注射液配合化疗治疗恶性肿瘤的临床观察.北京中医药 大学学报.1997,20(2) :50-51
[16] 陈良良,等.新加沙参麦冬汤治疗原发性肺癌的临床和实验研究.浙江 中医杂志.1997,(6) :247-248
[17] 韩明权,等.24味中药对人肺腺癌细胞核酸和蛋白质及细胞周期影响
的观察.中国中西医结合杂志.1995,15(3:147-149)
[18] 郭瑞林.扶正祛邪与肿瘤免疫.实用中西医结合杂志.1991,4:205
[19] 李家庚,等.中医肿瘤防治大全.北京:科学技术文献出版社,1994, 第1版:627. 607. 608. 587. 588
[20] 余桂清.恶性肿瘤中医治则治法研究进展,实用中西医结合杂志, 1991,4:205
[21] 唐文秀,等.中医药治疗原发性非小细胞肺癌临床观察中医杂志 1994,35(5) :284
[22] 郁仁存.中国肿瘤学(下册),北京:科学出版社,1985,第1版:147,204
[23] 潘敏求.中华肿瘤治疗大成.石家庄:河北科学技术出版社,1996,第1 版:55
[24] 王浴生.中药药理与应用,北京:人民卫生出版社,1983,第1版:326-330
[25] 雷海鹏,等.关于抗肿瘤药物的研究.药学学报.1063,(4) :199
[26] 赵锡民,等.清癌痛合复元汤治疗癌痛50例.山东中医杂志.1992;(5) : 20
[27] 李维廉,等.扶正女贞素对肿瘤放、化疗后患者免疫功能影响的临床研 究.全国第三届扶正培本防治研究学术研讨会论文汇编.1989:6-9
[28] 廖美琳.等.化疗在肺癌重的应用发展.见秦叔达.王建民,王杰军主 编.中国临床肿瘤学教育专辑(2001) .北京:中国医药科技出版社. 2001,12
[29] 杨宇飞,吴煜,姚晨.非小细胞肺癌中医临床研究方法探讨.见秦叔达, 王建民,王杰军主编.中国临床肿瘤学教育专辑(2001) .北京:中国 医药科技出版社.2001,61
[30] 王金荣,常春运.王知佳.扶正消积法治疗肺癌64例.辽宁中医杂志. 1996,23(1) :495
[31] 张珍玉.灵枢经语释,济南:山东科技出版社,1983,第1版:51
[32] 南京中医学院医学教研组.皇帝内经素问诊释,上海:上海科技出版社, 1961,第1版:122
[33] 周风梧,等.皇帝内经素问白话解,北京:人民卫生出版社,1958,第1 版:254
[34] 赵佶.圣济总录(上册),北京:人民卫生出版社,1962,第1版:1274
[35] 陈实功.外科正宗,上海:上海科学技术出版社,1989,第1版:326
[36] 张景岳.景岳全书,北京:人民卫生出版社,1991,第1版:354
[37] 魏鸿.医学实验动物学.成都:四川科技出版社,1998,423-427
[38] 姜泊,张亚历,周殿元.分子生物学常用实验方法.北京:人民军医出 版社,1996,103-162
[39] Harlow E, Williamson NM, Ralston R ,et al. Molecular cloning and in vitro expression of a cDNA clone for human cellnlar tumor antigen p53. Mol Cell Biol, 1985,5:1601-1610
[40] Serrano M, Hannon GL, Beach D. A new regulatory motif in cell-cycle control causing specific inhibition of cyclin D/CDK4. Nature, 1993,366:704-707
[41] 杨静平,孔玉英,林其谁.SA脂质体-高效介导DNA转染的新试剂.生 物化学与生物物理学报,1993,25:231-273
[42] 姜泊.细胞凋亡基础与临床.北京:人民军医出版社,1999,53
[43] 孙靖中,皱雄.肿瘤分子生物学.北京:人民卫生出版社,1998,119
[44] LaneDp. ADeathintheLifeofp53. Nature,1993;362(6423) : 7864
[45] LaneDp. p53,guardianoftheGenome.Nature,1992:358(6381) : 15-165
[46] 刘鸿君.p53基因突变与致癌作用.国外医学卫生学分 册,1996:23(2) :39