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首页> 外文期刊>DNA repair >MiR-375 targets the p53 gene to regulate cellular response to ionizing radiation and etoposide in gastric cancer cells
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MiR-375 targets the p53 gene to regulate cellular response to ionizing radiation and etoposide in gastric cancer cells

机译:MiR-375靶向p53基因以调节细胞对胃癌细胞中电离辐射和依托泊苷的反应

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摘要

MicroRNAs (miRNAs) offer a new approach for molecular classification and individual therapy of human cancer due to their regulation of oncogenic pathways. In a previous report, elevated miR-375 was found in recurring gastric cancer, and it was predicted that miR-375 may be a regulator of p53 gene. However, its biological role and mechanism of actions remain unknown. In this study, we characterized the expression level of miR-375 in gastric cancer cell lines - BGC823, MGC803, SGC7901, AGS, N87, MKN45 - using RT-PCR. We found that exogenous expression of miR-375 promoted the growth of AGS cells in both liquid and soft agar media. In agreement with the previous report, overexpression of miR-375 in AGS cells reduced the p53 protein expression level. A luciferase assay demonstrated that miR-375 down-regulated p53 expression through an interaction with the 3' UTR region of p53. In addition, the expression of miR-375 desensitizes cells to ionizing radiation and etoposide. Flow cytometry analyses showed that miR-375 abrogated the cell cycle arrest and apoptosis after DNA damage. These results demonstrate that miR-375 targets p53 to regulate the response to ionizing radiation and etoposide treatment.
机译:MicroRNA(miRNA)由于其对致癌途径的调控,为人类癌症的分子分类和个体治疗提供了一种新方法。在先前的报告中,在复发性胃癌中发现了miR-375升高,并且预测miR-375可能是p53基因的调节剂。但是,其生物学作用和作用机理仍然未知。在这项研究中,我们使用RT-PCR表征了miR-375在胃癌细胞系BGC823,MGC803,SGC7901,AGS,N87,MKN45中的表达水平。我们发现,miR-375的外源表达促进了液体和软琼脂培养基中AGS细胞的生长。与先前的报告一致,在AGS细胞中miR-375的过表达降低了p53蛋白的表达水平。萤光素酶试验证明,miR-375通过与p53的3'UTR区相互作用而下调了p53的表达。另外,miR-375的表达使细胞对电离辐射和依托泊苷不敏感。流式细胞仪分析表明,miR-375消除了DNA损伤后的细胞周期停滞和凋亡。这些结果证明,miR-375靶向p53来调节对电离辐射和依托泊苷治疗的反应。

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