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Hum Gene Ther. 2020 Oct;31(19-20):1074-1085. doi: 10.1089/hum.2019.169. Epub 2020 Jun 16.
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Cancer Biol Ther. 2020 Jun 2;21(6):477-485. doi: 10.1080/15384047.2020.1736482. Epub 2020 Mar 31.
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Cancer Biother Radiopharm. 2020 Jun;35(5):351-361. doi: 10.1089/cbr.2019.3120. Epub 2020 Mar 23.
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Mortal Obligate RNA Transcript Inhibits Cancer Cell Invasion and Migration in Lung Adenocarcinoma by Downregulating miRNA-223.致命必需 RNA 转录本通过下调 miRNA-223 抑制肺腺癌中的癌细胞侵袭和迁移。
Cancer Biother Radiopharm. 2020 Jun;35(5):345-350. doi: 10.1089/cbr.2019.3244. Epub 2020 Mar 11.
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2020: Gene Therapy Enters Its Fourth Decade.2020年:基因治疗进入第四个十年。
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Unexpected favorable outcome to etoposide and cisplatin in a small cell lung cancer transformed patient: a case report.依托泊苷和顺铂治疗小细胞肺癌转化患者获得意外良好结果:病例报告。
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携带生存素启动子的腺病毒载体传递的减毒白喉毒素对人肺癌细胞的治疗潜力。

The therapeutic potential of attenuated diphtheria toxin delivered by an adenovirus vector with survivin promoter on human lung cancer cells.

机构信息

Development and Regeneration Key Laboratory of Sichuan Province, Chengdu Medical College , Chengdu, China.

Department of Experiment Teaching Center of Clinical Medicine,Chengdu Medical College , Chengdu, China.

出版信息

Cancer Biol Ther. 2021 Jan 2;22(1):79-87. doi: 10.1080/15384047.2020.1859870. Epub 2020 Dec 30.

DOI:10.1080/15384047.2020.1859870
PMID:33377426
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7833756/
Abstract

Adenoviral vectors are superior to plasmid vectors in their gene transport efficiency. The A subunit of the diphtheria toxin (DTA) gene is a popular suicide gene in cancer gene therapy. However, DTA is seldom used in adenoviral therapy due to its great toxicity. The toxicity of DTA is so great that even a single molecule of DTA is enough to kill one cell. To avoid this highly toxic effect on normal cells, DTA should be controlled by tumor-specific promoters. The survivin promoter is a widely used tumor-specific promoter. But genes driven by the survivin promoter show a low level of basal gene expression in non-cancer cells. DTA driven by the survivin promoter in adenoviral vectors may be highly toxic not only to cancer cells but also to normal cells. Therefore, DTA should be attenuated when it is used in adenoviral vectors driven by the survivin promoter. In this study, we compared the three kinds of recombinant adenoviruses that carry DTA or its attenuated forms (DTA176 and DTA197) in the treatment of human lung cancer. The results showed that in comparison with both DTA and DTA176, DTA197 is more suitable for adenoviral cancer therapy controlled by the survivin promoter. In addition, Adsur-DTA197 (DTA197 delivered by an adenoviral vector with the survivin promoter) sensitized human lung cancer cells to cisplatin both and . These results indicated that Adsur-DTA197 may be a potential chemosensitizer in cancer therapy.

摘要

腺病毒载体在基因转导效率方面优于质粒载体。白喉毒素(DTA)基因的 A 亚基是癌症基因治疗中常用的自杀基因。然而,由于其毒性很大,DTA 很少用于腺病毒治疗。DTA 的毒性如此之大,以至于即使单个 DTA 分子也足以杀死一个细胞。为了避免对正常细胞产生这种高度毒性作用,DTA 应受肿瘤特异性启动子的控制。存活素启动子是一种广泛使用的肿瘤特异性启动子。但是,由存活素启动子驱动的基因在非癌细胞中表现出低水平的基础基因表达。腺病毒载体中由存活素启动子驱动的 DTA 不仅对癌细胞,而且对正常细胞可能具有高度毒性。因此,当 DTA 用于由存活素启动子驱动的腺病毒载体时,应使其减毒。在这项研究中,我们比较了携带 DTA 或其减毒形式(DTA176 和 DTA197)的三种重组腺病毒在人肺癌治疗中的作用。结果表明,与 DTA 和 DTA176 相比,DTA197 更适合由存活素启动子控制的腺病毒癌症治疗。此外,Adsur-DTA197(由携带存活素启动子的腺病毒载体传递的 DTA197)使人类肺癌细胞对顺铂更加敏感。这些结果表明,Adsur-DTA197 可能是癌症治疗中的一种有潜力的化疗增敏剂。