The Omicron XBB.1 Variant and Its Descendants: Genomic Mutations, Rapid Dissemination and Notable Characteristics

Author:

Giancotti Raffaele1ORCID,Lomoio Ugo1ORCID,Puccio Barbara1ORCID,Tradigo Giuseppe2ORCID,Vizza Patrizia1ORCID,Torti Carlo1ORCID,Veltri Pierangelo3ORCID,Guzzi Pietro Hiram1ORCID

Affiliation:

1. Department of Surgical and Medical Sciences, Magna Graecia University of Catanzaro, 88100 Catanzaro, Italy

2. SMARTEST Lab., eCampus University, 22060 Novedrate, Italy

3. Department of Computer Engineering, Modelling, Electronics and System, University of Calabria, 87036 Rende, Italy

Abstract

The SARS-CoV-2 virus, which is a major threat to human health, has undergone many mutations during the replication process due to errors in the replication steps and modifications in the structure of viral proteins. The XBB variant was identified for the first time in Singapore in the fall of 2022. It was then detected in other countries, including the United States, Canada, and the United Kingdom. We study the impact of sequence changes on spike protein structure on the subvariants of XBB, with particular attention to the velocity of variant diffusion and virus activity with respect to its diffusion. We examine the structural and functional distinctions of the variants in three different conformations: (i) spike glycoprotein in complex with ACE2 (1-up state), (ii) spike glycoprotein (closed-1 state), and (iii) S protein (open-1 state). We also estimate the affinity binding between the spike protein and ACE2. The market binding affinity observed in specific variants raises questions about the efficacy of current vaccines in preparing the immune system for virus variant recognition. This work may be useful in devising strategies to manage the ongoing COVID-19 pandemic. To stay ahead of the virus evolution, further research and surveillance should be carried out to adjust public health measures accordingly.

Funder

Regione Calabria proj Covid19@UMG Por Calabria

European Union

Relatech S.p.A.

Next Generation EU

Publisher

MDPI AG

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