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首页> 外文期刊>Cancer Cell International >MiR–20a-5p promotes radio-resistance by targeting Rab27B in nasopharyngeal cancer cells
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MiR–20a-5p promotes radio-resistance by targeting Rab27B in nasopharyngeal cancer cells

机译:MiR–20a-5p通过靶向Rab27B鼻咽癌细胞中的抗辐射性

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Background MicroRNAs (miRNAs) was reported to be involved in cancer radio-resistance, which remains a major obstacle for effective cancer therapy. Methods The differently expressed miRNAs were detected by RNA-seq experiment in nasopharyngeal cancer (NPC) cells. MiR-20a-5p was selected as our target, which was subject to finding its target gene Rab27B via bioinformatics analysis. The qRT-PCR, western blot and the luciferase reporter assays were performed to confirm Rab27B as the target of miR-20a-5p. In addition, the roles of miR-20a-5p in NPC radio-resistance were detected by transfection of either miR-20a-5p-mimic or miR-20a-5p-antagomiR. The involvement of Rab27B with NPC radio-resistance was also detected by the experiments with siRNA-mediated repression of Rab27B or over-expression of GFP-Rab27B. Wound healing and invasion assays were performed to detect the roles of both miR-20a-5p and Rab27B. Results MiR-20a-5p?promotes?NPC radio-resistance. We identified that its target gene Rab27B negatively correlates with miR-20a-5p-mediated NPC radio-resistance by systematic studies of a radio-sensitive (CNE-2) and resistant (CNE-1) NPC cell lines. Repression of Rab27B by siRNA suppresses cell apoptosis and passivates CNE-2 cells, whereas over-expression of Rab27B triggered cell apoptosis and sensitizes CNE-1 cells. Conclusions MiR-20a-5p and its target gene Rab27B might be involved in the NPC radio-resistance. Thus the key players and regulators involved in this pathway might be the potential targets for developing effective therapeutic strategies against NPC.
机译:背景技术据报道,MicroRNA(miRNA)参与了癌症的放射抗性,这仍然是有效癌症治疗的主要障碍。方法通过RNA-seq实验检测鼻咽癌(NPC)细胞中miRNA的表达差异。选择MiR-20a-5p作为我们的靶标,需要通过生物信息学分析找到其靶标基因Rab27B。进行qRT-PCR,蛋白质印迹和荧光素酶报告基因测定,以确认Rab27B为miR-20a-5p的靶标。此外,通过转染miR-20a-5p-mimic或miR-20a-5p-antagomiR可以检测到miR-20a-5p在NPC放射抗性中的作用。还通过siRNA介导的Rab27B抑制或GFP-Rab27B过表达的实验检测了Rab27B与NPC放射抗性的关系。进行伤口愈合和侵袭测定以检测miR-20a-5p和Rab27B的作用。结果MiR-20a-5p促进了NPC的抗辐射性。我们通过对放射敏感性(CNE-2)和耐药性(CNE-1)NPC细胞系进行系统研究,确定了其靶基因Rab27B与miR-20a-5p介导的NPC放射抗性负相关。 siRNA抑制Rab27B会抑制细胞凋亡并使钝化CNE-2细胞,而Rab27B的过表达会触发细胞凋亡并使CNE-1细胞敏感。结论MiR-20a-5p及其靶基因Rab27B可能参与了NPC的抗辐射性。因此,参与此途径的关键参与者和监管者可能是制定有效的针对NPC的治疗策略的潜在目标。

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