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Novel ACE2-IgG1 fusions with increased activity against SARS-CoV-2

biorxiv. 2020-06; 
Naoki?Iwanaga,?Laura?Cooper,?Lijun?Rong,?Brandon?Beddingfield,?Jackelyn?Crabtree,?Ralph A.?Tripp,??View ORCID ProfileJay K.?Kolls
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Gene Synthesis … The DNA sequences of the extracellular domains of ACE2 and IgG1 were synthesized by Genscript and cloned into pcDNA3.1. Transient transfection was performed using … Spike Glycoprotein Receptor Binding Domain (RBD) from SARS-Related Coronavirus 2 … Get A Quote

摘要

SARS-CoV2, the etiologic agent of COVID-19, uses ACE2 as a cell entry receptor. Soluble ACE2 has been shown to have neutralizing antiviral activity but has a short half-life and no active transport mechanism from the circulation into the alveolar spaces of the lung. To overcome this, we constructed an ACE2-human IgG1 fusion protein with mutations in the catalytic domain of ACE2. This fusion protein contained a LALA mutation that abrogates Fcrγ binding, but retains FcRN binding to prolong the half-life, as well as achieve therapeutic concentrations in the lung lavage. Interestingly, a mutation in the catalytic domain of ACE2, MDR504, completely abrogated catalytic activity, but significantly increased binding t... More

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