Author: Huang, Kuoâ€Yen; Lin, Mingâ€Shiu; Kuo, Tingâ€Chun; Chen, Ciâ€Ling; Lin, Chungâ€Chih; Chou, Yuâ€Chi; Chao, Taiâ€Ling; Pang, Yuâ€Hao; Kao, Hanâ€Chieh; Huang, Rihâ€Sheng; Lin, Steven; Chang, Suiâ€Yuan; Yang, Panâ€Chyr
Title: Humanized COVIDâ€19 decoy antibody effectively blocks viral entry and prevents SARSâ€CoVâ€2 infection Cord-id: gx8liztl Document date: 2020_11_30
ID: gx8liztl
Snippet: To circumvent the devastating pandemic caused by severe acute respiratory syndrome coronavirus 2 (SARSâ€CoVâ€2) infection, a humanized decoy antibody (ACE2â€Fc fusion protein) was designed to target the interaction between viral spike protein and its cellular receptor, angiotensinâ€converting enzyme 2 (ACE2). First, we demonstrated that ACE2â€Fc could specifically abrogate virus replication by blocking the entry of SARSâ€CoVâ€2 spikeâ€expressing pseudotyped virus into both ACE2â€express
Document: To circumvent the devastating pandemic caused by severe acute respiratory syndrome coronavirus 2 (SARSâ€CoVâ€2) infection, a humanized decoy antibody (ACE2â€Fc fusion protein) was designed to target the interaction between viral spike protein and its cellular receptor, angiotensinâ€converting enzyme 2 (ACE2). First, we demonstrated that ACE2â€Fc could specifically abrogate virus replication by blocking the entry of SARSâ€CoVâ€2 spikeâ€expressing pseudotyped virus into both ACE2â€expressing lung cells and lung organoids. The impairment of viral entry was not affected by virus variants, since efficient inhibition was also observed in six SARSâ€CoVâ€2 clinical strains, including the D614G variants which have been shown to exhibit increased infectivity. The preservation of peptidase activity also enables ACE2â€Fc to reduce the angiotensin IIâ€mediated cytokine cascade. Furthermore, this Fc domain of ACE2â€Fc was shown to activate NK cell degranulation after coâ€incubation with Spikeâ€expressing H1975 cells. These promising characteristics potentiate the therapeutic prospects of ACE2â€Fc as an effective treatment for COVIDâ€19.
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