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Multiple independent acquisitions of ACE2 usage in MERS-related coronaviruses

Cell. 2025-02; 
Cheng-Bao Ma, Chen Liu, Young-Jun Park, Jingjing Tang, Jing Chen, Qing Xiong, Jimin Lee, Cameron Stewart, Daniel Asarnow, Jack Brown, M Alejandra Tortorici, Xiao Yang, Ye-Hui Sun, Yuan-Mei Chen, Xiao Yu, Jun-Yu Si, Peng Liu, Fei Tong, Mei-Ling Huang, Jing Li, Zheng-Li Shi, Zengqin Deng, David Veesler, Huan Yan Wuhan University
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Codon Optimization Dimeric ACE2 ectodomain constructs were codon-optimized, synthesized, and inserted by Genscript into the pcDNA3.1(+) vector for the P.dav construct and pcDNA.3.4 vector for the P.nat constructs. Monomeric ACE2 constructs were codon-optimized, synthesized, and inserted into the pcDNA.3.4 vector by Genscript. RBD constructs were codon-optimized, synthesized, and inserted into the pcDNA3.1(+) vector by Genscript. Get A Quote

摘要

The angiotensin-converting enzyme 2 (ACE2) receptor is shared by various coronaviruses with distinct receptor-binding domain (RBD) architectures, yet our understanding of these convergent acquisition events remains elusive. Here, we report that two bat MERS-related coronaviruses (MERSr-CoVs) infecting Pipistrellus nathusii (P.nat)-MOW15-22 and PnNL2018B-use ACE2 as their receptor, with narrow ortholog specificity. Cryoelectron microscopy structures of the MOW15-22/PnNL2018B RBD-ACE2 complexes unveil an unexpected and entirely distinct binding mode, mapping >45 Å away from that of any other known ACE2-using coronaviruses. Functional profiling of ACE2 orthologs from 105 mammalian species led to the identificatio... More

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