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A new self-attenuated therapeutic influenza vaccine that uses host cell-restricted attenuation by artificial microRNAs

Int J Pharm. 2021-12; 
Ke Wen, Haiyan Wang, Yanping Chen, Huixiao Yang, Zhichao Zheng, Yongyong Yan, Realivazquez Adilene, Mingtao Zeng
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Gene Synthesis … All miRNAs and amiRNAs were engineered to encode cleavage sites for two endonucleases (Hpa I and Xho I), one at each end; synthesized by GenScript (Piscataway, NJ); and cloned into the microRNA-expressing plasmid pll3.7 to yield pll3.7-miR-30, pll3.7-amiR-30CLK1?… Get A Quote

摘要

New strategies are urgently needed for developing vaccines and/or anti-viral drugs against influenza viruses, because antigenic shift and drift inevitably occurs in circulating strains each year, and new strains resistant to anti-viral drugs have recently emerged. In our study, we designed and incorporated artificial microRNAs (amiRNAs) into the NA segment of rescued influenza viruses to separately target two host genes, Cdc2-like kinase 1 (CLK1) and SON DNA binding protein (SON), which were found to play an essential role in virus replication. Mouse epithelial fibroblast (MEF) or human lung carcinoma A549 cells infected with engineered influenza PR8 viruses expressing amiR-30CLK1 (PR8-amiR-30CLK1) or amiR-93SO... More

關鍵詞

Cdc2-like kinase 1, SON DNA-binding protein, artificial microRNA, intranasal delivery, live attenuated influenza vaccine, therapeutic vaccine
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