Close relatives of MERS-CoV in bats use ACE2 as their functional receptors

Author:

Xiong Qing,Cao LeiORCID,Ma Chengbao,Liu Chen,Si Junyu,Liu Peng,Gu Mengxue,Wang Chunli,Shi Lulu,Tong Fei,Huang Meiling,Li Jing,Zhao Chufeng,Shen ChaoORCID,Chen YuORCID,Zhao HuabinORCID,Lan KeORCID,Wang XiangxiORCID,Yan HuanORCID

Abstract

SummaryMiddle East Respiratory Syndrome coronavirus (MERS-CoV) and several bat coronaviruses employ Dipeptidyl peptidase-4 (DPP4) as their functional receptors1–4. However, the receptor for NeoCoV, the closest MERS-CoV relative yet discovered in bats, remains enigmatic5. In this study, we unexpectedly found that NeoCoV and its close relative, PDF-2180-CoV, can efficiently use some types of bat Angiotensin-converting enzyme 2 (ACE2) and, less favorably, human ACE2 for entry. The two viruses use their spikes’ S1 subunit carboxyl-terminal domains (S1-CTD) for high-affinity and species-specific ACE2 binding. Cryo-electron microscopy analysis revealed a novel coronavirus-ACE2 binding interface and a protein-glycan interaction, distinct from other known ACE2-using viruses. We identified a molecular determinant close to the viral binding interface that restricts human ACE2 from supporting NeoCoV infection, especially around residue Asp338. Conversely, NeoCoV efficiently infects human ACE2 expressing cells after a T510F mutation on the receptor-binding motif (RBM). Notably, the infection could not be cross-neutralized by antibodies targeting SARS-CoV-2 or MERS-CoV. Our study demonstrates the first case of ACE2 usage in MERS-related viruses, shedding light on a potential bio-safety threat of the human emergence of an ACE2 using “MERS-CoV-2” with both high fatality and transmission rate.

Publisher

Cold Spring Harbor Laboratory

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