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Structure of Venezuelan equine encephalitis virus with its receptor LDLRAD3

Bingting Ma, Cuiqing Huang, Jun Ma, Ye Xiang () and Xinzheng Zhang ()
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Bingting Ma: Tsinghua University
Cuiqing Huang: Chinese Academy of Sciences (CAS)
Jun Ma: Chinese Academy of Sciences (CAS)
Ye Xiang: Tsinghua University
Xinzheng Zhang: Chinese Academy of Sciences (CAS)

Nature, 2021, vol. 598, issue 7882, 677-681

Abstract: Abstract Venezuelan equine encephalitis virus (VEEV) is an enveloped RNA virus that causes encephalitis and potentially mortality in infected humans and equines1. At present, no vaccines or drugs are available that prevent or cure diseases caused by VEEV. Low-density lipoprotein receptor class A domain-containing 3 (LDLRAD3) was recently identified as a receptor for the entry of VEEV into host cells2. Here we present the cryo-electron microscopy structure of the LDLRAD3 extracellular domain 1 (LDLRAD3-D1) in complex with VEEV virus-like particles at a resolution of 3.0 Å. LDLRAD3-D1 has a cork-like structure and is inserted into clefts formed between adjacent VEEV E2–E1 heterodimers in the viral-surface trimer spikes through hydrophobic and polar contacts. Mutagenesis studies of LDLRAD3-D1 identified residues that are involved in the key interactions with VEEV. Of note, some of the LDLRAD3-D1 mutants showed a significantly increased binding affinity for VEEV, suggesting that LDLRAD3-D1 may serve as a potential scaffold for the development of inhibitors of VEEV entry. Our structures provide insights into alphavirus assembly and the binding of receptors to alphaviruses, which may guide the development of therapeutic countermeasures against alphaviruses.

Date: 2021
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DOI: 10.1038/s41586-021-03909-1

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