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用含有干扰素基因的腺病毒载体治疗人乳腺癌异种移植瘤,由于病毒溶瘤和基因治疗,肿瘤会迅速消退。

Treatment of a human breast cancer xenograft with an adenovirus vector containing an interferon gene results in rapid regression due to viral oncolysis and gene therapy.

作者信息

Zhang J F, Hu C, Geng Y, Selm J, Klein S B, Orazi A, Taylor M W

机构信息

Department of Biology, Indiana University, Bloomington 47405, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Apr 30;93(9):4513-8. doi: 10.1073/pnas.93.9.4513.

Abstract

Treatment of a human breast cancer cell line (MDA-MB-435) in nude mice with a recombinant adenovirus containing the human interferon (IFN) consensus gene, IFN-con1 (ad5/IFN), resulted in tumor regression in 100% of the animals. Tumor regression occurred when virus was injected either within 24 hr of tumor cell implantation or with established tumors. However, regression of the tumor was also observed in controls in which either the wild-type virus or a recombinant virus containing the luciferase gene was used, although tumor growth was not completely suppressed. Tumor regression was accompanied by a decrease in p53 expression. Two other tumors, the human myelogenous leukemic cell line K562 and the hamster melanoma tumor RPMI 1846, also responded to treatment but only with ad5/IFN. In the case of K562 tumors, there was complete regression of the tumor, and tumors derived from RPMI 1846 showed partial regression. We propose that the complete regression of the breast cancer with the recombinant virus ad5/IFN was the result of two events: viral oncolysis in which tumor cells are being selectively lysed by the replication-competent virus and the enhanced effect of expression of the IFN-con1 gene. K562 and RPMI 1846 tumors regressed only as a result of IFN gene therapy. This was confirmed by in vitro analysis. Our results indicate that a combination of viral oncolysis with a virus of low pathogenicity, itself resistant to the effects of IFN and IFN gene therapy, might be a fruitful approach to the treatment of a variety of different tumors, in particular breast cancers.

摘要

用含人干扰素(IFN)共有基因IFN-con1的重组腺病毒(ad5/IFN)处理裸鼠体内的人乳腺癌细胞系(MDA-MB-435),100%的动物出现肿瘤消退。在肿瘤细胞植入后24小时内注射病毒或对已形成的肿瘤注射病毒时,均会出现肿瘤消退。然而,在使用野生型病毒或含荧光素酶基因的重组病毒的对照组中也观察到了肿瘤消退,尽管肿瘤生长未被完全抑制。肿瘤消退伴随着p53表达的降低。另外两种肿瘤,即人髓性白血病细胞系K562和仓鼠黑色素瘤肿瘤RPMI 1846,也对治疗有反应,但仅对ad5/IFN有反应。就K562肿瘤而言,肿瘤完全消退,而源自RPMI 1846的肿瘤则出现部分消退。我们认为,重组病毒ad5/IFN使乳腺癌完全消退是两个事件的结果:病毒溶瘤,即有复制能力的病毒选择性地裂解肿瘤细胞;以及IFN-con1基因表达的增强作用。K562和RPMI 1846肿瘤仅因IFN基因治疗而消退。这一点通过体外分析得到了证实。我们的结果表明,将病毒溶瘤与低致病性病毒(其本身对IFN和IFN基因治疗的作用具有抗性)相结合,可能是治疗多种不同肿瘤,特别是乳腺癌的有效方法。

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