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机构地区:[1]武汉大学中南医院血液内科,湖北武汉430071
出 处:《现代肿瘤医学》2014年第3期489-493,共5页Journal of Modern Oncology
基 金:国家自然科学基金资助项目(编号:81001053);教育部直属高校专项科研基金武汉大学自主项目(编号:4101041)
摘 要:目的:观察PJ34对多发性骨髓瘤细胞株RPMI8226体外生长的影响以及与小剂量马法兰的协同作用,初步探讨其作用机制。方法:采用MTT法检测细胞增殖抑制率,Western blot方法检测FA/BRCA途径中的相关蛋白表达、流式细胞仪测定细胞周期及凋亡率。结果:PJ34能使细胞发生G2/M期阻滞、协同马法兰诱导细胞凋亡作用。PJ34与马法兰联用与单用马法兰相比,细胞凋亡率由(31.08±0.47)%增至(45.38±4.53)%。PJ34介导的FA/BRCA途径相关因子受抑制及γH2AX表达增强,从而抑制DNA的损伤修复。结论:PJ34对多发性骨髓瘤RPMI8226细胞有显著的抑制作用,并可增加RPMI8226细胞对烷化剂类化疗药物马法兰的敏感性,其作用机制可能是通过抑制FA/BRCA途径对DNA损伤的修复。PJ34与小剂量烷化剂化疗药物合用,是一种安全有效的逆转耐药的治疗方案。Objective:To observe the effects of PJ34 on MM cell line RPMI8226 and the synergetie effect with small doses of melphalan, and to explore its meehanisim. Methods:The inhibitory effects of the drugs on the growth of RPMI8226 cells were determined by MTT assay. The expression of FA/BRCA pathway related genes was determined by Western blot. Cell cycle phase was analysed by flow cytometry. Results: PJ34 - mediated inhibition of the related genes involved in FA/BRCA pathway and the enhanced expression of γH2AX gene,thereby inhibiting the DNA dam- age repair. P J34 can make cells have G2/M phase arrest,collaborate melphalan to induce cell apoptosis. The apoptosis percentage of RPMI8226 cells was significantly increased from (31.08± 0.47) % to (45.38 ± 4.53) % by the treat- ment of melphalan plus P J34. Conclusion: PJ34 can significantly inhibit human multiple myeloma cell line RP- Mi8226,and increase the sensitivity of RPMI8226 cells to alkylating agent chemotherapy drug melphalan,the inhibi- tion of FA/BRCA pathway may be the mechanism. PJ34 may be a safe reversal agent of drug resistance with low - dose alkylating agents.
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