The efficacy of TKIs in treatment of human primary small cell lung cancer xenograft model in vivo

doi:10.13459/j.cnki.cjap.2016.06.009

中国应用生理学杂志 ›› 2016, Vol. 32 ›› Issue (6): 525-528.doi: 10.13459/j.cnki.cjap.2016.06.009

The efficacy of TKIs in treatment of human primary small cell lung cancer xenograft model in vivo

Yu-hua ZHANG, Liang SUN, Bin LIU, Guo-qiang LI

Department of Respiratory and Intensive Care Unit, Affiliated Hospital of Logistics College of Chinese People's Armed Police Forces, Tianjin 300162, China

收稿日期:2016-08-20 修回日期:2016-11-21 出版日期:2016-11-28 发布日期:2018-06-19
通讯作者: Guo-qiang LI,MD,PhD,Department of Respiratory and Intensive Care Unit,Affiliated Hospital of Logistics College of Chinese People's Armed Police Forces,220 Chenglin Street,Hedong District,Tianjin 300162,China.Tel:86-22-60578941;E-mail:tjzyh1@126.com E-mail:tjzyh1@126.com

The efficacy of TKIs in treatment of human primary small cell lung cancer xenograft model in vivo

Yu-hua ZHANG, Liang SUN, Bin LIU, Guo-qiang LI

Department of Respiratory and Intensive Care Unit, Affiliated Hospital of Logistics College of Chinese People's Armed Police Forces, Tianjin 300162, China

Received:2016-08-20 Revised:2016-11-21 Online:2016-11-28 Published:2018-06-19

摘要/Abstract

摘要： Objective: To study the treatmaient of non-small cell lung cancer, we established the HU-Prim allograft transplantation tumor model. Methods: The fresh tumor samples were transplanted in the right scapular subcutaneous layer of the severe combined immunodeficient Non-obese diabetic/severe combined immunodeficient (NOD/SCID) mice. The pathological features of the tumors were observed. Nonnecrotic tissue was inoculated subcutaneously into the right axillary. When the tumor in burdened rat grew approximately 100 mm³, according to the tumor size all the animals were divided into the following four groups, eight rats in each group:solvent control group, gefitinib group (100 mg/kg), erlotinib group (50 mg/kg), afatinib group (20 mg/kg). Aniamals were treated with drugs by intragastric (i.g.) administrated, once daily, for consecutively 14 days. Measure the tumor size 2-3 times every week. Results: HuPrime1-NSCLC mutant sensitive xenograft model research data showed that reversible tyrosine kinase inhibitors gefitinib, erlotinib and irreversible tyrosine kinase inhibitor afatinib could effectively inhibit tumor growth in EGFR positive NSCLC allografts model. The pharmacodynamic activity of irreversible inhibitor was better than that of the reversible inhibitor. Specimens from clinical anthropogenic tumor retain characteristics of the human primary malignancy, histopathology, biological characteristics, and tumor markers, etc., which can more accurately reflect the characteristics of the tumor and the impact of interventions. Conclusion: The model is not only a good antitumor drug experimental platform, but also a new evaluation tool of individualized medication.

关键词: non-small-cell lung cancer (NSCLC), Non-obese diabetic/severe combined immunodeficient (NOD/SCID) mice, efficacy, tyrosine kinase inhibitors (TKIs), disease model

Abstract: Objective: To study the treatmaient of non-small cell lung cancer, we established the HU-Prim allograft transplantation tumor model. Methods: The fresh tumor samples were transplanted in the right scapular subcutaneous layer of the severe combined immunodeficient Non-obese diabetic/severe combined immunodeficient (NOD/SCID) mice. The pathological features of the tumors were observed. Nonnecrotic tissue was inoculated subcutaneously into the right axillary. When the tumor in burdened rat grew approximately 100 mm³, according to the tumor size all the animals were divided into the following four groups, eight rats in each group:solvent control group, gefitinib group (100 mg/kg), erlotinib group (50 mg/kg), afatinib group (20 mg/kg). Aniamals were treated with drugs by intragastric (i.g.) administrated, once daily, for consecutively 14 days. Measure the tumor size 2-3 times every week. Results: HuPrime1-NSCLC mutant sensitive xenograft model research data showed that reversible tyrosine kinase inhibitors gefitinib, erlotinib and irreversible tyrosine kinase inhibitor afatinib could effectively inhibit tumor growth in EGFR positive NSCLC allografts model. The pharmacodynamic activity of irreversible inhibitor was better than that of the reversible inhibitor. Specimens from clinical anthropogenic tumor retain characteristics of the human primary malignancy, histopathology, biological characteristics, and tumor markers, etc., which can more accurately reflect the characteristics of the tumor and the impact of interventions. Conclusion: The model is not only a good antitumor drug experimental platform, but also a new evaluation tool of individualized medication.

Key words: non-small-cell lung cancer (NSCLC), Non-obese diabetic/severe combined immunodeficient (NOD/SCID) mice, efficacy, tyrosine kinase inhibitors (TKIs), disease model

Yu-hua ZHANG, Liang SUN, Bin LIU, Guo-qiang LI. The efficacy of TKIs in treatment of human primary small cell lung cancer xenograft model in vivo[J]. 中国应用生理学杂志, 2016, 32(6): 525-528.

Yu-hua ZHANG, Liang SUN, Bin LIU, Guo-qiang LI. The efficacy of TKIs in treatment of human primary small cell lung cancer xenograft model in vivo[J]. CJAP, 2016, 32(6): 525-528.

参考文献

1. Jemal A, Bray F, Center MM, et al. Global cancer statistics[J]. CA Cancer J Clin, 2011, 61(2):69-90.
2. Favaretto AG, Pasello G, Magro C. Second and third line treatment in advanced non-small cell lung cancer[J]. Discov Med, 2009, 8(43):204-209.
3. Fichtner I, Rolff J, Soong R, et al. Establishment of patient-derived Non-small cell lung cancer xenografts as models for the identification of predictive biomarkers[J]. Clin Cancer Res, 2008, 14(20):6456-6468.
4. Fiebig HH, Dengler WA, Roth T. Human tumor xenografts:predictivity, and discovery of new anticancer agents[J]. Contrib Oncol.Basel Karger, 1999, 54:29-50.
5. Zhang XC. Primary lung cancer animal model of progress[J]. Evidence-Based Med, 2009, 9(4):195.
6. Perez-Soler R, Kemp B, Wu QP, et al. Response and determinants of sensitivity to paclitaxel in human non-small cell lung cancer tumors heterotransplanted in nude mice[J]. Clin Cancer Res, 2000, 6(12):4932-4938.
7. Fichtner I, Rolff J, Soong R, et al. Establishment of patient-derived non-small cell lung cancer xenografts as models for the identification of predictive biomarkers[J]. Clin Cancer Res, 2008, 14(20):6456-6468.
8. Bankert RB, Egilmez NK, Hess SD. Human-SCID mouse chimeric models for the evaluation of anti-cancer therapies[J]. Trends Immunol, 2001, 22(7):386-393.
9. Bankert RB, Hess SD, Egilmez NK. SCID mouse models to study human cancer pathogenesis and approaches to therapy:potential, limitations, and future directions[J]. Front Biosci, 2002, 7:c44-c62.
10. Dustin ML, de Fougerolles AR. Reprogramming T cells:the role of extracellular matrix in coordination of T cell activation and migration[J]. Curr Opin Immunol, 2001, 13(3):286-290.
11. Ibe S, Qin Z, Schuler T, et al. Tumor rejection by disturbing tumor stroma cell interactions[J]. J Exp Med, 2001, 194(11):1549-1559.
12. McCawley LJ, Matrisian LM. Tumor progression:defining the soil round the tumor seed[J]. Curr Biol, 2001, 11(1):R25-R27.
13. Tlsty TD. Stromal cell can contribute oncogenic signals[J]. Semin Cancer Biol, 2001, 11(2):97-104.

The efficacy of TKIs in treatment of human primary small cell lung cancer xenograft model in vivo

The efficacy of TKIs in treatment of human primary small cell lung cancer xenograft model in vivo

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