Evaluation of imatinib mesylate(Gleevec) on KAI1/CD82 gene expression in breast cancer MCF-7 cells using quantitative real-time PCR 被引量：1

Evaluation of imatinib mesylate(Gleevec) on KAI1/CD82 gene expression in breast cancer MCF-7 cells using quantitative real-time PCR

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摘要 Objective: To evaluate the effect of imatinib mesylate on cell viability, anti cancer effect through modulation of KAI1/CD82 gene expression in breast cancer MCF-7 cell line.Methods: The effects of imatinib mesylate on cell viability in MCF-7 cell line were assessed using MTT assay and IC_(50) value was determined. GAPDH and KAI1/CD82 were selected as reference and target genes, respectively. Quantitative real time PCR technique was applied for investigation of KAI1/CD82 gene expression in human breast cancer MCF-7 cells. Subsequently, the quantity of KAI1 compared to GAPDH gene expressions were analyzed using the formula; 2^(-DDCt).Results: Imatinib was showed to have a dose-dependent inhibitory effect on the viability of MCF-7 cells. CD82/GAPDH gene expression ratios were 1.322 ± 0.030(P > 0.05),2.052 ± 0.200(P < 0.05), 2.151 ± 0.270(P < 0.05) for 10, 20 and 40 mmol/L of imatinib concentrations.Conclusions: Based on the present data, imatinib mesylate might modulate metastasis by up-regulating KAI1/CD82 gene expression in human breast MCF-7 cancer cell line. Objective: To evaluate the effect of imatinib mesylate on cell viability, anti cancer effect through modulation of KAI1/CD82 gene expression in breast cancer MCF-7 cell line.Methods: The effects of imatinib mesylate on cell viability in MCF-7 cell line were assessed using MTT assay and IC_(50) value was determined. GAPDH and KAI1/CD82 were selected as reference and target genes, respectively. Quantitative real time PCR technique was applied for investigation of KAI1/CD82 gene expression in human breast cancer MCF-7 cells. Subsequently, the quantity of KAI1 compared to GAPDH gene expressions were analyzed using the formula; 2^(-DDCt).Results: Imatinib was showed to have a dose-dependent inhibitory effect on the viability of MCF-7 cells. CD82/GAPDH gene expression ratios were 1.322 ± 0.030(P > 0.05),2.052 ± 0.200(P < 0.05), 2.151 ± 0.270(P < 0.05) for 10, 20 and 40 mmol/L of imatinib concentrations.Conclusions: Based on the present data, imatinib mesylate might modulate metastasis by up-regulating KAI1/CD82 gene expression in human breast MCF-7 cancer cell line.

作者 Seyed Ataollah Sadat Shandiz Marjan Khosravani Sepideh Mohammadi Hassan Noorbazargan Amir Mirzaie Davoud Nouri Inanlou Mojgan Dalirsaber Jalali Hamidreza Jouzaghkar Fahimeh Baghbani-Arani Behta Keshavarz-Pakseresht

机构地区 Young Researchers and Elite Club Department of Microbiology Department of Microbiology Department of Biotechnology R&D Department Department of Microbiology Department of Genetics & Biotechnology

出处《Asian Pacific Journal of Tropical Biomedicine》 SCIE CAS 2016年第2期159-163,共5页 亚太热带生物医学杂志（英文版）

基金 Supported by East Tehran Branch,Islamic Azad University(Grant No.923064)

关键词 IMATINIB MESYLATE KAI1/CD82 METASTASIS BREAST cancer Real-time PCR Imatinib mesylate KAI1/CD82 Metastasis Breast cancer Real-time PCR

分类号 R737.9 [医药卫生—肿瘤]

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参考文献27

1Shweta Bansal.??Is imatinib still the best choice as first-line oral TKI(J)South Asian Journal of Cancer . 2014 (1) 被引量：1
2Jean-Yves Blay,Piotr Rutkowski.??Adherence to imatinib therapy in patients with gastrointestinal stromal tumors(J)Cancer Treatment Reviews . 2014 (2) 被引量：1
3Rebecca Siegel,Jiemin Ma,Zhaohui Zou,Ahmedin Jemal.Cancer statistics, 2014[J]. CA A Cancer Journal for Clinicians . 2014 (1) 被引量：48
4Aaron Rosenberg,Paul Mathew.??Imatinib and prostate cancer: lessons learned from targeting the platelet-derived growth factor receptor(J)Expert Opinion on Investigational Drugs . 2013 (6) 被引量：1
5Bruno F. Fernandes,Sebastian Di Cesare,Rubens Neto Belfort,Shawn Maloney,Claudia Martins,Enzo Castiglione,Jordan Isenberg,Daniel Abourbih,Emilia Antecka,Miguel N. Burnier Jr..??Imatinib mesylate alters the expression of genes related to disease progression in an animal model of uveal melanoma(J)Analytical Cellular Pathology . 2011 (3) 被引量：1
6Hiroshi Haeno,Franziska Michor.??The evolution of tumor metastases during clonal expansion(J)Journal of Theoretical Biology . 2009 (1) 被引量：1
7Marion T. Weigel,Ivo Meinhold-Heerlein,Dirk O. Bauerschlag,Christian Schem,Maret Bauer,Walter Jonat,Nicolai Maass,Christoph Mundhenke.??Combination of imatinib and vinorelbine enhances cell growth inhibition in breast cancer cells via PDGFR β signalling(J)Cancer Letters . 2008 (1) 被引量：1
8Bo Keun Jee,Joo Yong Lee,Young Lim,Kweon Haeng Lee,Yang-Hyeok Jo.??Effect of KAI1/CD82 on the β1 integrin maturation in highly migratory carcinoma cells(J)Biochemical and Biophysical Research Communications . 2007 (3) 被引量：1
9Bozdogan O,Yulug G,Vargel I,Cavusoglu T,Karabulut A,Karahan G,et al.Differential expression pattern of metastasis suppressor proteins in basal cell carcinoma. International Journal of Dermatology . 2015 被引量：1
10Saad Zaghloul MA,Abadi AH,Abdelaziz AI.Functional evaluation of imatinib mesylate in hepatocellular carcinoma cells. Recent Pat Biomark . 2013 被引量：1

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1Ourlad Alzeus G.Tantengco,Sonia D.Jacinto.Cytotoxic activity of crude extracts and fractions from Premna odorata(Blanco),Artocarpus camansi(Blanco) and Gliricidia sepium(Jacq.) against selected human cancer cell lines[J].Asian Pacific Journal of Tropical Biomedicine,2015,5(12):1037-1041.
2Mohamed Saleh Abdelfattah,Mohammed Ismail Youssef Elmallah,Usama Wahid Hawas,Lamia Taha Abou El-Kassema,Mennat Allah Gamal Eid.Isolation and characterization of marine-derived actinomycetes with cytotoxic activity from the Red Sea coast[J].Asian Pacific Journal of Tropical Biomedicine,2016,6(8):651-657. 被引量：3
3Jose Manuel Lorenzo,Paulo Eduardo Sichetti Munekata.Phenolic compounds of green tea: Health benefits and technological application in food[J].Asian Pacific Journal of Tropical Biomedicine,2016,6(8):709-719. 被引量：9
4韩芸,王强.Id-2在结直肠癌组织中的表达及临床意义[J].海南医学,2016,27(14):2246-2248. 被引量：1
5杨微,张丹凤,李梅秀,卢北燕,朴英兰,王丽新,马宝红.肿瘤转移抑制基因KAI1/CD82及骨桥蛋白OPN在妊娠滋养细胞疾病中的表达[J].黑龙江医药科学,2015,38(6):63-64. 被引量：3
6马燕,赵建美.P27^(kip1)、Jab1、Skp2的生物学功能及其与非霍奇金淋巴瘤发生、发展关系的研究进展[J].山东医药,2015,55(28):108-110. 被引量：2
7金菲,陈易,徐华,张国新.胃癌患者癌组织HIF-1α、TGF-β共表达及其临床意义[J].山东医药,2015,55(44):54-56.
8吴霜霜,戚益铭,冯波,沈敏鹤.姜黄素抗原发性肝癌的实验研究进展[J].生物技术世界,2014,11(12):131-132. 被引量：1
9张鹏江,崔曼莉,张超,王景杰,张明鑫.炎症相关细胞因子对食管癌细胞株miR-302b表达的影响[J].现代肿瘤医学,2016,24(5):690-693. 被引量：3
10李彦姝,汤丽娜,张红艳,高云凌,李丰.CUEDC2通过上皮-间质转化促进人乳腺癌MCF-7细胞侵袭转移[J].现代肿瘤医学,2016,24(11):1681-1683. 被引量：6

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1李嘉玮,耿雪,张新宇,陈星宇,阚玉萍,侯雪,刘爽,王维维,阎雪莹.熊果酸/PF127/TPGS-多柔比星纳米胶束对HepG-2/ADR细胞增殖和凋亡的影响及其体内药动学研究[J].华西药学杂志,2023,38(5):521-525. 被引量：1

1刘达人,曹利平.胃肠道间质瘤的治疗进展[J].国际消化病杂志,2006,26(5):303-306.
2王利华,阎超,李烿烿,路伟.预照射联合siRNA抑制小鼠肺癌Survivin基因表达的研究[J].中国癌症杂志,2015,25(5):339-344.
3吕转,李砺锋,范智蕊,马望,王留兴.干细胞基因Lgr5在食管鳞癌组织中的表达及其临床意义[J].肿瘤防治研究,2016,43(10):863-869. 被引量：6
4Halaven获批治疗晚期乳腺癌[J].中国处方药,2010(12):60-60.
5于飞（译）.FDA批准晚期乳腺癌药Halaven[J].药品评价,2010(22):47-47.
6胡乃刚,周荣祥,陈强.塞来昔布对前列腺癌细胞株PC-3中VEGF-C及bcl-2 mRNA表达的影响[J].肿瘤防治研究,2008,35(4):233-235. 被引量：2
7肖卫群.THE EXPRESSION OF CDK4 GENE IN HUMAN BREAST CANCER[J].Chinese Journal of Cancer Research,1997,9(2):107-110.
8Chunyou Cai Zhi Yao.Activation of NF-κB in Human Breast Cancer and its Role in Cell Proliferation and Progresssion[J].Chinese Journal of Clinical Oncology,2006,3(1):5-10. 被引量：4
9张焕新.Effect of VE-cadherin on sentitivity to Imatinib in Sup-B15 Philadelphia chromosome positive acute lymphoblastic leukemia cells[J].China Medical Abstracts(Internal Medicine),2013,30(3):184-184.
10胡维新,曾赵军,罗赛群,陈迁.Suicide gene therapy of human breast cancer in SCID mice model by the regulation of Tet-On[J].Chinese Medical Journal,2004(3):434-439. 被引量：7

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