Identification of Evolutionary Trajectories Shared across Human Betacoronaviruses

Author:

Escalera-Zamudio Marina12ORCID,Kosakovsky Pond Sergei L3ORCID,Martínez de la Viña Natalia1,Gutiérrez Bernardo12ORCID,Inward Rhys P D1ORCID,Thézé Julien4ORCID,van Dorp Lucy5ORCID,Castelán-Sánchez Hugo G26ORCID,Bowden Thomas A7ORCID,Pybus Oliver G18ORCID,Hulswit Ruben J G7ORCID

Affiliation:

1. Department of Biology, University of Oxford , Oxford , United Kingdom

2. Consorcio Mexicano de Vigilancia Genómica (CoViGen-Mex) , Mexico City , Mexico

3. Department of Biology, Institute for Genomics and Evolutionary Medicine, Temple University , Philadelphia, PA 19122 , USA

4. Epidemiology of Animal and Zoonotic Diseases, UMR 0346, INRAE, VetAgroSup , Saint-Gènes-Champanelle , France

5. Department of Genetics, Evolution and Environment, UCL Genetics Institute, University College London , London , United Kingdom

6. Programa de Investigadoras e Investigadores por México, Consejo Nacional de Ciencia y Tecnología , Mexico City , México

7. Division of Structural Biology, Wellcome Centre for Human Genetics, University of Oxford , Oxford , United Kingdom

8. Department of Pathobiology, Royal Veterinary College , London , United Kingdom

Abstract

Abstract Comparing the evolution of distantly related viruses can provide insights into common adaptive processes related to shared ecological niches. Phylogenetic approaches, coupled with other molecular evolution tools, can help identify mutations informative on adaptation, although the structural contextualization of these to functional sites of proteins may help gain insight into their biological properties. Two zoonotic betacoronaviruses capable of sustained human-to-human transmission have caused pandemics in recent times (SARS-CoV-1 and SARS-CoV-2), although a third virus (MERS-CoV) is responsible for sporadic outbreaks linked to animal infections. Moreover, two other betacoronaviruses have circulated endemically in humans for decades (HKU1 and OC43). To search for evidence of adaptive convergence between established and emerging betacoronaviruses capable of sustained human-to-human transmission (HKU1, OC43, SARS-CoV-1, and SARS-CoV-2), we developed a methodological pipeline to classify shared nonsynonymous mutations as putatively denoting homoplasy (repeated mutations that do not share direct common ancestry) or stepwise evolution (sequential mutations leading towards a novel genotype). In parallel, we look for evidence of positive selection and draw upon protein structure data to identify potential biological implications. We find 30 candidate mutations, from which 4 (codon sites 18121 [nsp14/residue 28], 21623 [spike/21], 21635 [spike/25], and 23948 [spike/796]; SARS-CoV-2 genome numbering) further display evolution under positive selection and proximity to functional protein regions. Our findings shed light on potential mechanisms underlying betacoronavirus adaptation to the human host and pinpoint common mutational pathways that may occur during establishment of human endemicity.

Publisher

Oxford University Press (OUP)

Subject

Genetics,Ecology, Evolution, Behavior and Systematics

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