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Crystal structure of the receptor binding domain of the spike glycoprotein of human betacoronavirus HKU1.

Nat Commun. 2017; 
OuXiuyuan,GuanHongxin,QinBo,MuZhixia,WojdylaJustyna A,WangMeitian,DominguezSamuel R,QianZhaohui,CuiS
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Gene Synthesis The full-length, codon-optimized genotype A HKU1 spike gene (Accession #: AY597011) preceded by a Kozak sequence was synthesized by GenScript (Piscataway, NJ) and cloned into pcDNA3.1(þ) (Invitrogen) between HindIII and XbaI sites for eukaryotic expression. . Codon-optimized genotype B HKU1 S1 gene (Access#: AGT17758.1) preceded by a Kozak sequence (Supplementary Table 2) was also synthesized by GenScript (Piscataway, NJ) and cloned into pcDNA3.1 (pcDNAHKU1B S1). Get A Quote

摘要

Human coronavirus (CoV) HKU1 is a pathogen causing acute respiratory illnesses and so far little is known about its biology. HKU1 virus uses its S1 subunit C-terminal domain (CTD) and not the N-terminal domain like other lineage A β-CoVs to bind to its yet unknown human receptor. Here we present the crystal structure of HKU1 CTD at 1.9 Å resolution. The structure consists of three subdomains: core, insertion and subdomain-1 (SD-1). While the structure of the core and SD-1 subdomains of HKU1 are highly similar to those of other β-CoVs, the insertion subdomain adopts a novel fold, which is largely invisible in the cryo-EM structure of the HKU1 S trimer. We identify five residues in the insertion subdom... More

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