An extended conformation of SARS-CoV-2 main protease reveals allosteric targets.
Zengchao SunLu WangXiyang LiCheng-Peng FanJianfeng XuZhenzhong ShiHuarui QiaoZhongyun LanXin ZhangLingyun LiXin ZhouYong GengPublished in: Proceedings of the National Academy of Sciences of the United States of America (2022)
SignificanceThe coronavirus main protease (M pro ) is required for viral replication. Here, we obtained the extended conformation of the native monomer of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) M pro by trapping it with nanobodies and found that the catalytic domain and the helix domain dissociate, revealing allosteric targets. Another monomeric state is termed compact conformation and is similar to one protomer of the dimeric form. We designed a Nanoluc Binary Techonology (NanoBiT)-based high-throughput allosteric inhibitor assay based on structural conformational change. Our results provide insight into the maturation, dimerization, and catalysis of the coronavirus M pro and pave a way to develop an anticoronaviral drug through targeting the maturation process to inhibit the autocleavage of M pro .