丙酮酸乙酯联合顺铂作用裸鼠肝移植瘤的研究
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摘要
目的:研究丙酮酸乙酯(EP)与顺铂(CDDP)联合处理裸鼠对裸鼠肝癌HepG2移植瘤的作用效果,及对个体的副作用;方法:为裸鼠接种p-Gluc荧光标记的HepG2细胞,分为PBS处理组、CDDP(9.6mM)与EP(60μg)单独注射组、CDDP与EP联合注射组;对各组裸鼠的个体体重、移植瘤体积进行观察测量;结果:药物联合组的肿瘤体积显著小于对照组(*P=0.0146),而CDDP处理组无显著变化。药物联合组与CDDP组中肿瘤抑制率分别为36.8%和62.9%;药物联合组体重平均为21g,CDDP组为19g,EP组与对照组约为25g;结论:EP是CDDP增效剂,药物联合处理有望为肝癌治疗方案提出新的思路,并可能缓解化疗药物单独使用带来的副作用。
Objective:To study the effect of ethyl pyruvate(EP) combined with cisplatin(CDDP) on HepG2 transplanted tumor in nude mice and the side effects on individuals; Method:Inoculating p-Gluc fluorescently labeled HepG2 cells into nude mice,then divided into PBS-treated group, CDDP(9.6 mM) and EP(60 μg) Separate injection group, and CDDP-EP combined injection group; Observing and measuring individual body weight and transplanted tumor volume of each group; Results:The tumor volume of CDDP-EP therapy group was significantly smaller than that of the control group(*P =0.0146), while there was no significant change in the CDDP therapy group. The tumor inhibition rates in CDDP-EP therapy group and the CDDP group were36.8% and 62.9%, respectively; the average body weight of CDDP-EP therapy group was 21 g, the CDDP group was 19 g, while the EP group and the control group were nearly 25 g;Conclusion:EP is a CDDP synergist, the drug combination therapy is expected to provide new ideas for the treatment of liver cancer, and may alleviate the side effects caused by the separate use of chemotherapy drugs.
Objective:To study the effect of ethyl pyruvate(EP) combined with cisplatin(CDDP) on HepG2 transplanted tumor in nude mice and the side effects on individuals; Method:Inoculating p-Gluc fluorescently labeled HepG2 cells into nude mice,then divided into PBS-treated group, CDDP(9.6 mM) and EP(60 μg) Separate injection group, and CDDP-EP combined injection group; Observing and measuring individual body weight and transplanted tumor volume of each group; Results:The tumor volume of CDDP-EP therapy group was significantly smaller than that of the control group(*P =0.0146), while there was no significant change in the CDDP therapy group. The tumor inhibition rates in CDDP-EP therapy group and the CDDP group were36.8% and 62.9%, respectively; the average body weight of CDDP-EP therapy group was 21 g, the CDDP group was 19 g, while the EP group and the control group were nearly 25 g;Conclusion:EP is a CDDP synergist, the drug combination therapy is expected to provide new ideas for the treatment of liver cancer, and may alleviate the side effects caused by the separate use of chemotherapy drugs.
引文
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[2]彭芳华,马玄,邱丽美等.姜黄素增加HepG2细胞对顺铂敏感性的作用及机制研究[J].肿瘤药学,2016,6(2):120-125.
[3]Treutiger CJ,Mullins GE,Johansson AS,et al.High mobility group 1 B-box mediates activation of human endothelium[J].J Intern Med,2003,254(4):375-385.
[4]徐洪君,孟艳,孙宇新.人参皂苷Rh2联合顺铂应用对人喉癌细胞Hep-2的作用[J].中国实验诊断学,2005,9(4):584-587.
[5]栾正刚.高迁移率族蛋白B1在重症急性胰腺炎内皮细胞活化及肠粘膜损害中的作用[D].沈阳:中国医科大学,2008.
[6]梁勋.高迁移率族蛋白B1在严重烧伤延迟复苏大鼠急性肺损伤中的作用和初步机制[D].合肥:安徽医科大学,2012.
[7] Hu W,Liu PY,Yang YC,et al.Association of HMGB1 Gene Polymorphisms with Lung Cancer Susceptibility and Clinical Aspects[J].Send to Int J Med Sci,2017,14(12):1197-1202.
[8] Min Jiang,Xuelian Li,Xiaowei Quan,et al.Single Nucleotide Polymorphisms in HMGB1 Correlate with Lung Cancer Risk in the Northeast Chinese Han Population[J].Molecules,2018,23(4):832.
[9]DongXda E,Ito N,Lotze MT,et al.High mobility group box I(HMGB1)release from tumor cells after treatment:implications for development of targeted chemoimmunotherapy[J].J Immunother,2007,30(6):596-606.
[10]Ellerman JE,Brown CK,De Vera M,et al.Masquerader:high mobility group box-1 and cancer[J].Clin Cancer Res,2007,13(10):2836-2848.
[11]胡秋芳.高迁移率族蛋白B1的研究进展[J].科学与财富,2015,(6):64.
[12]方传勤.脑缺血再灌注DNA损伤与XRCC1的修复及褪黑素干预作用[D].重庆:第三军医大学,2004.
[13]Xiaohong Pan,Xiaoxiao Song,Cheng Wang,et al.H2Se Induces Reductive Stress in HepG2 Cells and Activates Cell Autophagy by Regulating the Redox of HMGB1 Protein under Hypoxia[J].Theranostics,2019,9(6):1794-1808.
[14]Luo F,Sun Z,Han Q,et al.Effect of Human Hepatocellular Carcinoma HepG2 Cell-derived Exosome on the Differentiation of Mesenchymal Stem Cells and Their Interaction[J].Zhongguo Yi Xue Ke Xue Yuan Xue Bao.2017,39(3):312-317.
[15] Choi JM1, Oh SJ, Lee SY,et al. HepG2 cells as an in vitro model for evaluation of cytochrome P450 induction by xenobiotics[J]. Arch Pharm Res,2015,38(5):691-704.
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