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Distinct antigenic properties of the SARS-CoV-2 Omicron lineages BA.4 and BA.5

View ORCID ProfileBrian J. Willett, View ORCID ProfileAshwini Kurshan, View ORCID ProfileNazia Thakur, Joseph Newman, Maria Manali, View ORCID ProfileGrace Tyson, Nicola Logan, View ORCID ProfilePablo R. Murcia, View ORCID ProfileLuke B. Snell, View ORCID ProfileJonathan D. Edgeworth, View ORCID ProfileJie Zhou, View ORCID ProfileKsenia Sukhova, Gayatri Amirthalingam, View ORCID ProfileKevin Brown, View ORCID ProfileBryan Charleston, View ORCID ProfileMichael H. Malim, View ORCID ProfileEmma C. Thomson, View ORCID ProfileWendy S. Barclay, View ORCID ProfileDalan Bailey, View ORCID ProfileKatie J. Doores, View ORCID ProfileThomas P. Peacock
doi: https://doi.org/10.1101/2022.05.25.493397
Brian J. Willett
1MRC-University of Glasgow Centre for Virus Research, Glasgow, UK
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Ashwini Kurshan
2Department of Infectious Diseases, School of Immunology & Microbial Sciences, King’s College London; London, UK
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Nazia Thakur
3The Pirbright Institute, Woking, Surrey, UK
4Nuffield Department of Medicine, The Jenner Institute, Oxford, UK
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Joseph Newman
3The Pirbright Institute, Woking, Surrey, UK
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Maria Manali
1MRC-University of Glasgow Centre for Virus Research, Glasgow, UK
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Grace Tyson
1MRC-University of Glasgow Centre for Virus Research, Glasgow, UK
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Nicola Logan
1MRC-University of Glasgow Centre for Virus Research, Glasgow, UK
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Pablo R. Murcia
1MRC-University of Glasgow Centre for Virus Research, Glasgow, UK
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Luke B. Snell
5Centre for Clinical Infection and Diagnostics Research, Department of Infectious Diseases, Guy’s and St Thomas’ NHS Foundation Trust; London, UK
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Jonathan D. Edgeworth
5Centre for Clinical Infection and Diagnostics Research, Department of Infectious Diseases, Guy’s and St Thomas’ NHS Foundation Trust; London, UK
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Jie Zhou
6Department of Infectious Diseases, Imperial College London, UK
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Ksenia Sukhova
6Department of Infectious Diseases, Imperial College London, UK
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Gayatri Amirthalingam
7Immunisation and Vaccine Preventable Diseases Division, UKHSA
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Kevin Brown
7Immunisation and Vaccine Preventable Diseases Division, UKHSA
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Bryan Charleston
3The Pirbright Institute, Woking, Surrey, UK
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Michael H. Malim
2Department of Infectious Diseases, School of Immunology & Microbial Sciences, King’s College London; London, UK
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Emma C. Thomson
1MRC-University of Glasgow Centre for Virus Research, Glasgow, UK
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Wendy S. Barclay
6Department of Infectious Diseases, Imperial College London, UK
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Dalan Bailey
3The Pirbright Institute, Woking, Surrey, UK
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Katie J. Doores
2Department of Infectious Diseases, School of Immunology & Microbial Sciences, King’s College London; London, UK
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Thomas P. Peacock
6Department of Infectious Diseases, Imperial College London, UK
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  • For correspondence: thomas.peacock09@imperial.ac.uk
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Abstract

Over the course of the pandemic variants have arisen at a steady rate. The most recent variants to emerge, BA.4 and BA.5, form part of the Omicron lineage and were first found in Southern Africa where they are driving the current wave of infection.

In this report, we perform an in-depth characterisation of the antigenicity of the BA.4/BA.5 Spike protein by comparing sera collected post-vaccination, post-BA.1 or BA.2 infection, or post breakthrough infection of vaccinated individuals with the Omicron variant. In addition, we assess sensitivity to neutralisation by commonly used therapeutic monoclonal antibodies.

We find sera collected post-vaccination have a similar ability to neutralise BA.1, BA.2 and BA.4/BA.5. In contrast, in the absence of vaccination, prior infection with BA.2 or, in particular, BA.1 results in an antibody response that neutralises BA.4/BA.5 poorly. Breakthrough infection with Omicron in vaccinees leads to a broad neutralising response against the new variants. The sensitivity of BA.4/BA.5 to neutralisation by therapeutic monoclonal antibodies was similar to that of BA.2.

These data suggest BA.4/BA.5 are antigenically distinct from BA.1 and, to a lesser extent, BA.2. The enhanced breadth of neutralisation observed following breakthrough infection with Omicron suggests that vaccination with heterologous or multivalent antigens may represent viable strategies for the development of cross-neutralising antibody responses.

Competing Interest Statement

The authors have declared no competing interest.

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 4.0 International license.
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Posted May 25, 2022.
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Distinct antigenic properties of the SARS-CoV-2 Omicron lineages BA.4 and BA.5
Brian J. Willett, Ashwini Kurshan, Nazia Thakur, Joseph Newman, Maria Manali, Grace Tyson, Nicola Logan, Pablo R. Murcia, Luke B. Snell, Jonathan D. Edgeworth, Jie Zhou, Ksenia Sukhova, Gayatri Amirthalingam, Kevin Brown, Bryan Charleston, Michael H. Malim, Emma C. Thomson, Wendy S. Barclay, Dalan Bailey, Katie J. Doores, Thomas P. Peacock
bioRxiv 2022.05.25.493397; doi: https://doi.org/10.1101/2022.05.25.493397
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Distinct antigenic properties of the SARS-CoV-2 Omicron lineages BA.4 and BA.5
Brian J. Willett, Ashwini Kurshan, Nazia Thakur, Joseph Newman, Maria Manali, Grace Tyson, Nicola Logan, Pablo R. Murcia, Luke B. Snell, Jonathan D. Edgeworth, Jie Zhou, Ksenia Sukhova, Gayatri Amirthalingam, Kevin Brown, Bryan Charleston, Michael H. Malim, Emma C. Thomson, Wendy S. Barclay, Dalan Bailey, Katie J. Doores, Thomas P. Peacock
bioRxiv 2022.05.25.493397; doi: https://doi.org/10.1101/2022.05.25.493397

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