Selection Analysis Identifies Clusters of Unusual Mutational Changes in Omicron Lineage BA.1 That Likely Impact Spike Function | Zendy

Darren P. Martin | Zendy; Spyros Lytras | Zendy; Alexander G. Lucaci | Zendy; Wolfgang Maier | Zendy; Björn Grüning | Zendy; Stephen D. Shank | Zendy; Steven Weaver | Zendy; Oscar A. MacLean | Zendy; Richard Orton | Zendy; Philippe Lemey | Zendy; Maciej F. Boni | Zendy; Houriiyah Tegally | Zendy; Gordon W. Harkins | Zendy; Cathrine Scheepers | Zendy; Jinal N. Bhiman | Zendy; Josie Everatt | Zendy; Daniel G. Amoako | Zendy; James Emmanuel San | Zendy; Jennifer Giandhari | Zendy; Alex Sigal | Zendy; Carolyn Williamson | Zendy; Marvin Hsiao | Zendy; Anne von Gottberg | Zendy; Arné de Klerk | Zendy; Robert W. Shafer | Zendy; David L. Robertson | Zendy; Robert J. Wilkinson | Zendy; B.T. Sewell | Zendy; Richard Lessells | Zendy; Anton Nekrutenko | Zendy; Allison J. Greaney | Zendy; Tyler N. Starr | Zendy; Jesse D. Bloom | Zendy; Ben Murrell | Zendy; Eduan Wilkinson | Zendy; Ravindra K. Gupta | Zendy; Túlio de Oliveira | Zendy; Sergei L. Kosakovsky Pond | Zendy

Open Access

Selection Analysis Identifies Clusters of Unusual Mutational Changes in Omicron Lineage BA.1 That Likely Impact Spike Function

Author(s) -

Darren P. Martin,

Spyros Lytras,

Alexander G. Lucaci,

Wolfgang Maier,

Björn Grüning,

Stephen D. Shank,

Steven Weaver,

Oscar A. MacLean,

Richard Orton,

Philippe Lemey,

Maciej F. Boni,

Houriiyah Tegally,

Gordon W. Harkins,

Cathrine Scheepers,

Jinal N. Bhiman,

Josie Everatt,

Daniel G. Amoako,

James Emmanuel San,

Jennifer Giandhari,

Alex Sigal,

Carolyn Williamson,

Marvin Hsiao,

Anne von Gottberg,

Arné de Klerk,

Robert W. Shafer,

David L. Robertson,

Robert J. Wilkinson,

B.T. Sewell,

Richard Lessells,

Anton Nekrutenko,

Allison J. Greaney,

Tyler N. Starr,

Jesse D. Bloom,

Ben Murrell,

Eduan Wilkinson,

Ravindra K. Gupta,

Túlio de Oliveira,

Sergei L. Kosakovsky Pond

Publication year - 2022

Publication title -

molecular biology and evolution

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 6.637

H-Index - 218

eISSN - 1537-1719

pISSN - 0737-4038

DOI - 10.1093/molbev/msac061

Subject(s) - biology , nonsynonymous substitution , genetics , mutation , lineage (genetic) , gene , selection (genetic algorithm) , negative selection , function (biology) , evolutionary biology , genome , computer science , artificial intelligence

Among the 30 nonsynonymous nucleotide substitutions in the Omicron S-gene are 13 that have only rarely been seen in other SARS-CoV-2 sequences. These mutations cluster within three functionally important regions of the S-gene at sites that will likely impact (1) interactions between subunits of the Spike trimer and the predisposition of subunits to shift from down to up configurations, (2) interactions of Spike with ACE2 receptors, and (3) the priming of Spike for membrane fusion. We show here that, based on both the rarity of these 13 mutations in intrapatient sequencing reads and patterns of selection at the codon sites where the mutations occur in SARS-CoV-2 and related sarbecoviruses, prior to the emergence of Omicron the mutations would have been predicted to decrease the fitness of any virus within which they occurred. We further propose that the mutations in each of the three clusters therefore cooperatively interact to both mitigate their individual fitness costs, and, in combination with other mutations, adaptively alter the function of Spike. Given the evident epidemic growth advantages of Omicron overall previously known SARS-CoV-2 lineages, it is crucial to determine both how such complex and highly adaptive mutation constellations were assembled within the Omicron S-gene, and why, despite unprecedented global genomic surveillance efforts, the early stages of this assembly process went completely undetected.

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