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miRNA-200c对非小细胞肺癌A549细胞甲氨蝶呤耐药性的影响
引用本文:单武林,邓芳,张晓蕾,张婧,韩丹丹,万玲玲,李明. miRNA-200c对非小细胞肺癌A549细胞甲氨蝶呤耐药性的影响[J]. 肿瘤防治研究, 2016, 43(5): 321-325. DOI: 10.3971/j.issn.1000-8578.2016.05.001
作者姓名:单武林  邓芳  张晓蕾  张婧  韩丹丹  万玲玲  李明
作者单位:230031 合肥,安徽省肿瘤医院(安徽省立医院西区)检验科
基金项目:安徽省自然科学基金(1308085QH144)
摘    要:目的 探讨miRNA-200c(miR-200c)在非小细胞肺癌A549细胞耐甲氨蝶呤(MTX)(A549/MTX)中的影响及可能的作用机制。方法 通过实时荧光定量(qRT-PCR)法检测人肺癌亲本细胞株A549细胞、转染miR-200c模拟物(mimic)的A549/MTX细胞(A549/MTX-M)及转染miR- 阴性对照(NC)A549/MTX细胞(A549/MTX-N)中miR-200c的表达水平。分别采用MTT法、锥虫兰染色及流式细胞术检测三组细胞对MTX的药物敏感度、细胞增殖能力及细胞凋亡变化,并采用qRT-PCR检测其P53和P21基因表达的变化。结果 miR-200c在A549细胞中的表达水平显著高于A549/MTX-N细胞;A549/MTX-M细胞miR-200c水平高于A549/MTX-N细胞;用不同浓度MTX刺激细胞,与A549/MTX-N细胞比较,A549/MTX-M细胞的增殖能力减弱、凋亡细胞增多,并呈剂量依赖性,差异均有统计学意义。转染miR-200c mimic后,P53和P21基因表达水平上升,与转染miR-NC细胞比较,差异有统计学意义。结论 miR-200c能够逆转A549/MTX细胞对MTX的耐药性,其作用机制可能是通过P53/P21信号转导通路诱导细胞凋亡来实现的。

关 键 词:miR-200c  甲氨蝶呤  耐药  肺癌  
收稿时间:2015-05-29

Impact of miRNA-200c on Methotrexate Resistance of Non-small Cell Lung Cancer Cells A549
SHAN Wulin,DENG Fang,ZHANG Xiaolei,ZHANG Jing,HAN Dandan,WAN Lingling,LI Ming. Impact of miRNA-200c on Methotrexate Resistance of Non-small Cell Lung Cancer Cells A549[J]. Cancer Research on Prevention and Treatment, 2016, 43(5): 321-325. DOI: 10.3971/j.issn.1000-8578.2016.05.001
Authors:SHAN Wulin  DENG Fang  ZHANG Xiaolei  ZHANG Jing  HAN Dandan  WAN Lingling  LI Ming
Affiliation:Department of Clinical Laboratory, Anhui Provincial Cancer Hospital (West Branch of Anhui Provincial Hospital), Hefei 230031, China
Abstract:Objective To explore the effect of microRNA-200c (miR-200c) on methotrexate (MTX) resistance of non-small cell lung cancer cells A549 (A549/MTX) and elucidate its related mechanism. Methods Quantitative real-time PCR (qRT-PCR) was used to detect the miR-200c expression in A549 cells, A549/MTX cells transfected with miR-200c mimic (A549/MTX-M) and A549/MTX cells transfected with miR-negative control (A549/MTX-N). MTT assay, Trypan blue staining and flow cytometry analysis were sequentially performed to detect the sensitivity of A549, A549/MTX-M and A549/MTX-N cells to MTX, cell proliferation and apoptosis. qRT-PCR was used to detect the gene expressions of P53 and P21 in these cells. Results The miR-200c expression in A549 cells was significantly higher than that in A549/MTX-N cells. The miR-200c expression in A549/MTX-M cells was significantly higher than that in A549/MTX-N cells. Compared with A549/MTX-N cells, the proliferation inhibition and apoptosis of A549/MTX-M cells were increased after treated with MTX in a concentration-dependent manner, with significant difference. Furthermore, the up-regulated P53 and P21 expression were observed in A549/MTX-M cells, with significant difference compared with A549/MTX-N cells(P=0.023, P=0.015). Conclusion miR-200c could reduce the resistance of A549/MTX cells to MTX with the possible mechanism of inducing the apoptosis through the P53/P21 pathway.
Keywords:MicroRNA-200c(miR-200c)  Methotrexate(MTX)  Drug resistance  Lung cancer  
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