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Non-small cell lung cancers (NSCLCs) oncolysis using coxsackievirus B5 and synergistic DNA-damage response inhibitors

Signal Transduct Target Ther. 2023-09; 
Bopei Cui, Lifang Song, Qian Wang, Kelei Li, Qian He, Xing Wu, Fan Gao, Mingchen Liu, Chaoqiang An, Qiushuang Gao, Chaoying Hu, Xiaotian Hao, Fangyu Dong, Jiuyue Zhou, Dong Liu, Ziyang Song, Xujia Yan ,,Jialu Zhang, Yu Bai, Qunying Mao, Xiaoming Yang, Zhenglun Liang
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Gene Services The backbone plasmids lenti-sgRNA and lenti-cas9-zeocin were obtained from GenScript Co., Ltd. (Nanjing, China). sgRNA (AATTCCCACAAGGACAAAAG) was designed and subcloned into the cas9 backbone. Lucia luciferase reporter HEK293cells were first infected with lenti-cas9-zeocin and then selected using zeocin. The stable sublines were then infected with lenti-sgRNA to specifically knock out the target genes. Get A Quote

摘要

With the continuous in-depth study of the interaction mechanism between viruses and hosts, the virus has become a promising tool in cancer treatment. In fact, many oncolytic viruses with selectivity and effectiveness have been used in cancer therapy. Human enterovirus is one of the most convenient sources to generate oncolytic viruses, however, the high seroprevalence of some enteroviruses limits its application which urges to exploit more oncolytic enteroviruses. In this study, coxsackievirus B5/Faulkner (CV-B5/F) was screened for its potential oncolytic effect against non-small cell lung cancers (NSCLCs) through inducing apoptosis and autophagy. For refractory NSCLCs, DNA-dependent protein kinase (DNA-PK) or ... More

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