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作 者:彭利[1] 刘涛[2] 张青云[3] 张萌[1] 王顺祥[1] 唐瑞峰[1] 张凤瑞[1]
机构地区:[1]河北医科大学第四医院肝胆外科,石家庄050011 [2]济宁医学院附属医院肝胆血管外科,济宁272029 [3]承德医学院附属医院普外二科,承德067000
出 处:《肿瘤》2007年第5期361-364,共4页Tumor
基 金:河北省卫生厅医学科学研究重点课题计划项目(编号:05138)
摘 要:目的:观察survivin反义寡核苷酸(ASODN)对SMMC-7721细胞增殖、凋亡的影响及其对化疗药物敏感性的作用。方法:设计合成特异性survivin的ASODN,脂质体转染肝细胞癌SMMC-7721细胞,透射电镜观察细胞超微结构变化;RT-PCR法检测survivin mRNA的表达变化;FCM法检测对细胞周期、凋亡及survivin蛋白表达的影响;MTT法测定survivin表达抑制前后细胞对吡柔比星、氟苷、顺铂敏感性的影响。结果:ASODN转染后细胞呈现凋亡的形态学改变,survivin mRNA和蛋白表达减弱(P<0.05),诱导SMMC-7721细胞凋亡(P<0.01),细胞周期阻滞于G2/M期(P<0.05)。ASODN转染组可增加SMMC-7721细胞对吡柔比星、氟苷、顺铂的敏感性(P<0.01)。结论:Survivin ASODN转染能下调survivin表达,诱导SMMC-7721细胞凋亡,提高对吡柔比星、氟苷、顺铂的敏感性。Objective:To observe the effect of antisense oligonucleotide (ASODN) targeting survivin on apoptosis, proliferation and sensitivity to chemotherapeutic agents of hepatocellular carcinoma cell line SMMC-7721. Methods: Specific ASODN targeting survivin was designed and constructed, and transfected into SMMC-7721 cells mediated by oligofectamine. Cell morphological changes were examined by transmission electron microscopy. The expression of survivin mRNA was detected by RT-PCR. Cell cycle, apoptosis and the expression of survivin protein were detected by flow cytometry. Changes of sensitivity to pirarubicin, doxifluridine, and cisplatin of SMMC-7721 cells were detected by MTT assay. Results: Morphological abnormalities of cells were observed in ASODN transfected groups. The mRNA and protein expressions of survivin were significantly decreased compared with that of control group (P 〈 0.05 ). The transfection of survivin ASODN induced significant apoptosis (P 〈 0.01 ) and increased the proportion of cells in the G2/M phase(P 〈 0.05 ). Compared with that in control group, oligofectamine group and SODN groups, the sensitivity of ASODN groups to pirarubicin, doxifluridine, and cisplatin were significantly enhanced (P 〈 0.01 ). Conclusion: The transfection of survivin ASODN down-regulated the mRNA and protein expressions of survivin, induces apoptosis, and enhances its sensitivity to pirarubicin, doxifluridine, and cisplatin of SMMC-7721 cells.
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