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携带可溶性转化生长因子-β受体II与人免疫球蛋白Fc融合蛋白的溶瘤腺病毒用于乳腺癌治疗的研发。

Development of oncolytic adenovirus armed with a fusion of soluble transforming growth factor-beta receptor II and human immunoglobulin Fc for breast cancer therapy.

作者信息

Seth Prem, Wang Zhen-Guo, Pister Amanda, Zafar M Behzad, Kim Sung, Guise Theresa, Wakefield Lalage

机构信息

Gene Therapy Program, Evanston Northwestern Healthcare Research Institute and Department of Medicine, Evanston Hospital, Northwestern University, Evanston, IL 60201, USA.

出版信息

Hum Gene Ther. 2006 Nov;17(11):1152-60. doi: 10.1089/hum.2006.17.1152.

DOI:10.1089/hum.2006.17.1152
PMID:17032151
Abstract

We have developed an approach to cancer gene therapy in which the oncolytic effects of an adenoviral vector have been combined with selective expression of a soluble form of transforming growth factor (TGF)-beta receptor II fused with Fc (sTGFbetaRIIFc). We chose to use adenoviral dl01/07 mutant because it can replicate in all cancer cells regardless of their genetic defects. An oncolytic adenovirus expressing sTGFbetaRIIFc (Ad.sT- betaRFc) was constructed by homologous recombination. Infection of MDA-MB-231 and MCF-7 human breast cancer cells with Ad.sTbetaRFc produced sTGFbetaRIIFc, which was released into the media. The conditioned media containing sTGFbetaRIIFc could bind with TGF-beta 1 and inhibited TGF-beta-dependent transcription in target cells. Infection of MDA-MB-231, MCF-7, and 76NE human breast cancer cells with Ad.sTbetaRFc resulted in high levels of viral replication, comparable to that of a wild-type dl309 virus. Although some viral replication was observed in actively dividing normal human lung fibroblasts, there was no replication in nonproliferating normal cells. Direct injection of Ad.sTbetaRFc into MDA-MB-231 human breast xenograft tumors grown in nude mice resulted in a significant inhibition of tumor growth, causing tumor regression in more than 85% of the animals. These results indicate that it is possible to construct an oncolytic virus expressing sTGFbetaRIIFc in which both viral replication and transgene expression remain intact, and the recombinant adenovirus is oncolytic in a human tumor xenograft model. On the basis of these results we believe that it may be feasible to develop a cancer gene therapy approach using Ad.sTbetaRFc as an antitumor agent.

摘要

我们已经开发出一种癌症基因治疗方法,其中腺病毒载体的溶瘤作用与可溶性形式的转化生长因子(TGF)-β受体II与Fc融合体(sTGFβRIIFc)的选择性表达相结合。我们选择使用腺病毒dl01/07突变体,因为它可以在所有癌细胞中复制,而不论其基因缺陷如何。通过同源重组构建了表达sTGFβRIIFc的溶瘤腺病毒(Ad.sT-βRFc)。用Ad.sTβRFc感染MDA-MB-231和MCF-7人乳腺癌细胞产生了sTGFβRIIFc,其被释放到培养基中。含有sTGFβRIIFc的条件培养基可以与TGF-β1结合并抑制靶细胞中TGF-β依赖性转录。用Ad.sTβRFc感染MDA-MB-231、MCF-7和76NE人乳腺癌细胞导致高水平的病毒复制,与野生型dl309病毒相当。虽然在活跃分裂的正常人肺成纤维细胞中观察到一些病毒复制,但在非增殖正常细胞中没有复制。将Ad.sTβRFc直接注射到裸鼠体内生长的MDA-MB-231人乳腺异种移植肿瘤中导致肿瘤生长的显著抑制,使超过85%的动物肿瘤消退。这些结果表明,有可能构建一种表达sTGFβRIIFc的溶瘤病毒,其中病毒复制和转基因表达均保持完整,并且重组腺病毒在人肿瘤异种移植模型中具有溶瘤作用。基于这些结果,我们认为使用Ad.sTβRFc作为抗肿瘤剂开发一种癌症基因治疗方法可能是可行的。

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