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

Cancer Biol Ther. 2020-12; 
Lvxia Dai, Xiaoping Yu, Sizhou Huang, Yanjuan Peng, Jianmin Liu, Tian Chen, Xin Wang, Qiaofeng Liu, Yanfeng Zhu, Dengbang Chen, Xiaohua Li, Yu Ou, Yi Zou, Qu Pan, Kang Cao
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Codon Optimization … The mutant human EF-2 gene (G to R at codon 717) was chemically synthesized (by GenScript) and inserted into the lentiviral vector plasmid pCDH-CMV-MCS-EF1-copGFP-T2A-Puro (System Biosciences) at the EcoRI site and the BamHI site. This recombinant lentiviral vector … Get A Quote

摘要

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 t... More

關鍵詞

DTA, DTA176, DTA197, adenoviruses, lung cancer, survivin promoter
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