SARS-CoV-2 Mutant Spectra As Variant of Concern Nurseries: Endless Variation?

Overview

Journal Front Microbiol

Specialty Microbiology

Date 2024 Apr 1

PMID 38559344

Authors

Brenda Martinez-Gonzalez

Maria Eugenia Soria

Pablo Minguez

Ramon Lorenzo-Redondo

Llanos Salar-Vidal

Alberto Lopez-Garcia

Mario Esteban-Munoz

Antoni Duran-Pastor

Pilar Somovilla

Carlos Garcia-Crespo

Ana Isabel de Avila

Jordi Gomez

Jaime Esteban

Ricardo Fernandez-Roblas

Ignacio Gadea

Esteban Domingo

Celia Perales

Affiliations

Soon will be listed here.

Abstract

Introduction: SARS-CoV-2 isolates of a given clade may contain low frequency genomes that encode amino acids or deletions which are typical of a different clade.

Methods: Here we use high resolution ultra-deep sequencing to analyze SARS-CoV-2 mutant spectra.

Results: In 6 out of 11 SARS-CoV-2 isolates from COVID-19 patients, the mutant spectrum of the spike (S)-coding region included two or more amino acids or deletions, that correspond to discordant viral clades. A similar observation is reported for laboratory populations of SARS-CoV-2 USA-WA1/2020, following a cell culture infection in the presence of remdesivir, ribavirin or their combinations. Moreover, some of the clade-discordant genome residues are found in the same haplotype within an amplicon.

Discussion: We evaluate possible interpretations of these findings, and reviewed precedents for rapid selection of genomes with multiple mutations in RNA viruses. These considerations suggest that intra-host evolution may be sufficient to generate minority sequences which are closely related to sequences typical of other clades. The results provide a model for the origin of variants of concern during epidemic spread─in particular Omicron lineages─that does not require prolonged infection, involvement of immunocompromised individuals, or participation of intermediate, non-human hosts.

Citing Articles

A general and biomedical perspective of viral quasispecies.

Domingo E, Martinez-Gonzalez B, Somovilla P, Garcia-Crespo C, Soria M, de Avila A RNA. 2024; 31(3):429-443.

PMID: 39689947 PMC: 11874995. DOI: 10.1261/rna.080280.124.

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