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腺相关病毒载体转导的p21WAF1/CIP1基因启动子的低剂量辐射反应

Low-dose radiation response of the p21WAF1/CIP1 gene promoter transduced by adeno-associated virus vector.

作者信息

Nenoi Mitsuru, Daino Kazuhiro, Ichimura Sachiko, Takahash Shin-ichiro, Akuta Teruo

机构信息

Radiation Effect Mechanisms Research Group, National Institute of Radiological Sciences, 9-1, Anagawa-4-chome, Inage-ku, Chiba 263-8555, Japan.

出版信息

Exp Mol Med. 2006 Oct 31;38(5):553-64. doi: 10.1038/emm.2006.65.

Abstract

In cancer gene therapy, restriction of antitumor transgene expression in a radiation field by use of ionizing radiation-inducible promoters is one of the promising approaches for tumor-specific gene delivery. Although tumor suppressor protein p53 is induced by low doses (< 1 Gy) of radiation, there have been only a few reports indicating potential utilization of a p53-target gene promoter, such as that of the p21 gene. This is mainly because the transiently transfected promoter of p53-target genes is not much sensitive to radiation. We examined the response of the p21 gene promoter to low-dose radiation when transduced into a human breast cancer cell line MCF-7 by use of recombinant adeno-associated virus (rAAV) vectors. It was shown that the p21 gene promoter transduced by rAAV vectors was more highly radiation-responsive than that transiently transfected by electroporation. A significant induction of the p21 gene promoter by radiation of low doses down to 0.2 Gy was observed. When cells were transduced with the p21 gene promoter-driven HSVtk gene by rAAV vector, they were significantly sensitized to repetitive treatment with low dose radiation (1 Gy) in the presence of the prodrug ganciclovir. It was therefore considered that the p21 gene promoter in combination with a rAAV vector is potentially usable for the development of a low-dose radiation-inducible vector for cancer gene therapy.

摘要

在癌症基因治疗中,利用电离辐射诱导型启动子将抗肿瘤转基因表达限制在辐射场内是肿瘤特异性基因递送的一种有前景的方法。尽管肿瘤抑制蛋白p53可由低剂量(<1 Gy)辐射诱导,但仅有少数报告表明p53靶基因启动子(如p21基因启动子)具有潜在利用价值。这主要是因为p53靶基因的瞬时转染启动子对辐射不太敏感。我们利用重组腺相关病毒(rAAV)载体将p21基因启动子导入人乳腺癌细胞系MCF-7,检测其对低剂量辐射的反应。结果表明,rAAV载体转导的p21基因启动子比电穿孔瞬时转染的启动子对辐射的反应性更高。观察到低至0.2 Gy的低剂量辐射可显著诱导p21基因启动子。当用rAAV载体将p21基因启动子驱动的HSVtk基因导入细胞时,在存在前体药物更昔洛韦的情况下,它们对低剂量辐射(1 Gy)的重复治疗显著敏感。因此,认为p21基因启动子与rAAV载体联合使用有可能用于开发癌症基因治疗的低剂量辐射诱导载体。

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