Five‐Year (2017–2022) Evolutionary Dynamics of Human Coronavirus HKU1 in Southern France With Emergence of Viruses Harboring Spike H512R Substitution

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Hikmat, Houmadi | Le Targa, Lorlane | Boschi, Céline | Py, Justine | Morand, Aurélie | Lagier, Jean‐christophe | Aherfi, Sarah | Fantini, Jacques | La Scola, Bernard | Colson, Philippe

Edité par CCSD ; Wiley-Blackwell -

International audience. ABSTRACT HCoV‐HKU1 diversity and evolution were scarcely studied. We performed next‐generation sequencing (NGS) and analysis of HCoV‐HKU1 genomes over 5 years. NGS used Illumina technology on NovaSeq 6000 following whole genome PCR amplification by an in‐house set of primers designed using Gemi and PrimalScheme. Genome assembly and analyses used CLC Genomics, Mafft, BioEdit, Nextstrain, Nextclade, MEGA, and iTol bioinformatic tools. Spike molecular modeling and dynamics simulations used Molegro Molecular Viewer and Hyperchem programs. Twenty‐eight PCR systems allowed obtaining 158 HCoV‐HKU1 genomes including 69 and 89 of genotypes A and B, respectively. Both genotypes co‐circulated during the study period but one predominated each year. A total of 1683 amino acid substitutions including 80 in ≥ 10 genomes were detected in genotype A relatively to a 2004 reference. H512R in spike, first detected in 2009 and reported as involved in antibody neutralization, was found in all genotype A, almost always with V387I and K478N, and was predicted here to significantly improve cellular TMPRSS2 protein binding. Also, 1802 amino acid substitutions including 64 in ≥ 10 genomes were detected in genotype B relatively to a 2005 reference. This study substantially expands the global set of HCoV‐HKU1 genomes. Genomics with protein structural analyses contributed to our understanding of HCoV‐HKU1 evolution.

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