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Putative APOBEC3 deaminase editing in MPXV as evidence for sustained human transmission since at least 2016

View ORCID ProfileÁine O’Toole, View ORCID ProfileRichard A. Neher, Nnaemeka Ndodo, View ORCID ProfileVitor Borges, Ben Gannon, View ORCID ProfileJoão Paulo Gomes, Natalie Groves, David J King, Daniel Maloney, View ORCID ProfilePhilippe Lemey, Kuiama Lewandowski, Nicholas Loman, Richard Myers, View ORCID ProfileMarc A. Suchard, Michael Worobey, Meera Chand, Chikwe Ihekweazu, David Ulaeto, Ifedayo Adetifa, Andrew Rambaut
doi: https://doi.org/10.1101/2023.01.23.525187
Áine O’Toole
1Institute of Ecology & Evolution, University of Edinburgh, Edinburgh, EH9 3FL, United Kingdom
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  • For correspondence: aine.otoole@ed.ac.uk a.rambaut@ed.ac.uk
Richard A. Neher
2Biozentrum, University of Basel and Swiss Institute of Bioinformatics, Switzerland
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Nnaemeka Ndodo
3Nigeria Centers for Disease Control and Prevention, Abuja, Nigeria
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Vitor Borges
4National Institute of Health Doutor Ricardo Jorge, Lisbon, Portugal
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Ben Gannon
5UK Health Security Agency, Porton Down, Salisbury, United Kingdom
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João Paulo Gomes
4National Institute of Health Doutor Ricardo Jorge, Lisbon, Portugal
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Natalie Groves
6UK Health Security Agency, London, SW1P 3HX, United Kingdom
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David J King
7Defence Science and Technology Laboratory (DSTL), Chemical, Biological and Radiological Division, Porton Down, Salisbury, United Kingdom
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Daniel Maloney
1Institute of Ecology & Evolution, University of Edinburgh, Edinburgh, EH9 3FL, United Kingdom
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Philippe Lemey
8Department of Microbiology, Immunology and Transplantation, Rega Institute, KU Leuven – University of Leuven, Belgium
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Kuiama Lewandowski
5UK Health Security Agency, Porton Down, Salisbury, United Kingdom
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Nicholas Loman
6UK Health Security Agency, London, SW1P 3HX, United Kingdom
9University of Birmingham, Birmingham, United Kingdom
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Richard Myers
6UK Health Security Agency, London, SW1P 3HX, United Kingdom
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Marc A. Suchard
10Department of Biostatistics, Fielding School of Public Health, University of California, Los Angeles, USA
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Michael Worobey
11Department of Ecology and Evolutionary Biology, University of Arizona, USA
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Meera Chand
6UK Health Security Agency, London, SW1P 3HX, United Kingdom
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Chikwe Ihekweazu
3Nigeria Centers for Disease Control and Prevention, Abuja, Nigeria
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David Ulaeto
7Defence Science and Technology Laboratory (DSTL), Chemical, Biological and Radiological Division, Porton Down, Salisbury, United Kingdom
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Ifedayo Adetifa
3Nigeria Centers for Disease Control and Prevention, Abuja, Nigeria
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Andrew Rambaut
1Institute of Ecology & Evolution, University of Edinburgh, Edinburgh, EH9 3FL, United Kingdom
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  • For correspondence: aine.otoole@ed.ac.uk a.rambaut@ed.ac.uk
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Abstract

Mpox is often described as being endemic in West and Central Africa as a zoonotic disease that transmits through contact with the reservoir rodent host, likely a species of African squirrel. In May 2022, human cases of Mpox were detected spreading internationally beyond countries with known endemic reservoirs. At time of writing, 84,700 confirmed cases have been reported in 110 countries. When the first cases from 2022 were sequenced, it was seen that they shared 42 single nucleotide differences from the closest mpox virus (MPXV) genome sampled in 2018. This number of changes within 3-4 years is unexpectedly large and points to a much greater evolutionary rate than expected for a poxvirus. Strikingly, most nucleotide changes are of a specific type – a dinucleotide change from TC->TT or its reverse complement GA->AA. This mutation type is characteristic of the action of APOBEC3 deaminases; host-enzymes with reported antiviral function. Analysis of MPXV genomes sampled from 2017 to 2022 showed further evidence of TC->TT mutation pattern enrichment, with 93% of transmitted single nucleotide mutations since 2017 consistent with APOBEC3 editing. Assuming APOBEC-editing is characteristic of MPXV infection in human hosts, we propose an APOBEC clock that – at a rate of ~6 APOBEC3 mutations per year – estimates MPXV has been circulating in humans since 2016. This evolutionary pattern of host-enzyme editing has implications for the longer-term fitness of the virus in this epidemic as such mechanisms are primarily antiviral in function, but in the context of a poxvirus also provide a source of variation that may conceivably facilitate adaptation.

Competing Interest Statement

The authors have declared no competing interest.

Footnotes

  • ↵† these authors are joint-senior

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. It is made available under a CC-BY-NC-ND 4.0 International license.
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Posted January 24, 2023.
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Putative APOBEC3 deaminase editing in MPXV as evidence for sustained human transmission since at least 2016
Áine O’Toole, Richard A. Neher, Nnaemeka Ndodo, Vitor Borges, Ben Gannon, João Paulo Gomes, Natalie Groves, David J King, Daniel Maloney, Philippe Lemey, Kuiama Lewandowski, Nicholas Loman, Richard Myers, Marc A. Suchard, Michael Worobey, Meera Chand, Chikwe Ihekweazu, David Ulaeto, Ifedayo Adetifa, Andrew Rambaut
bioRxiv 2023.01.23.525187; doi: https://doi.org/10.1101/2023.01.23.525187
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Putative APOBEC3 deaminase editing in MPXV as evidence for sustained human transmission since at least 2016
Áine O’Toole, Richard A. Neher, Nnaemeka Ndodo, Vitor Borges, Ben Gannon, João Paulo Gomes, Natalie Groves, David J King, Daniel Maloney, Philippe Lemey, Kuiama Lewandowski, Nicholas Loman, Richard Myers, Marc A. Suchard, Michael Worobey, Meera Chand, Chikwe Ihekweazu, David Ulaeto, Ifedayo Adetifa, Andrew Rambaut
bioRxiv 2023.01.23.525187; doi: https://doi.org/10.1101/2023.01.23.525187

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