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A novel biparatopic antibody-ACE2 fusion that blocks SARS-CoV-2 infection: implications for therapy

biorxiv. 2020-06; 
Xiaoniu Miao,,Yi Luo, Xi Huang, Suki M. Y. Lee,Zhijun Yuan,Yongzhou Tang,Liandi Chen,Chao Wang,Wenchao Jiang,Wei Gao, Xuedong Song,Yao Yan,Tuling Pang,Yuefeng Zou,Weihui Fu,Liping Wan,Javier Gilbert-Jaramillo,Michael Knight,Tiong Kit Tan,Pramila Rijal,Alain Townsend,Joanne Sun,Xiaolin Liu,William James,Andy Tsun,Yingda Xu
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Recombinant Proteins  Transfected cells were incubated for 7 days at 37 °C. IgG in the supernatants were purified for by Protein A magnetic beads (Genscript) according to manufacturer’s instructions. Get A Quote

摘要

In the absence of a proven effective vaccine preventing infection by SARS-CoV-2, or a proven drug to treat COVID-19, the positive results of passive immune therapy using convalescent serum provides a strong lead. We have developed a new class of tetravalent, biparatopic therapy, 89C8-ACE2. It combines the specificity of a monoclonal antibody (89C8) that recognizes the relatively conserved N-terminal domain (NTD) of the viral S glycoprotein, and the ectodomain of ACE2, which binds to the receptor-binding domain (RBD) of S. This molecule shows exceptional performance in vitro, inhibiting the interaction of recombinant S1 to ACE2 and transduction of ACE2-overexpressing cells by S-pseudotyped lentivirus with IC50s ... More

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