Structural epitope profiling identifies antibodies associated with critical COVID-19 and long COVID

Author:

Kearns Patrick KA12ORCID,Dixon Charles1,Badonyi Mihaly1ORCID,Lee Kim3,Czapiewski Rafal1,Fleming Olivia1,Nadukkandy Prajitha3,Gerasimivicius Lukas1,Sahputra Rinal4,Potts Bethany4,Benton Sam3,Guy Jacky5ORCID,Neilson Scott6,Wise Helen7ORCID,Jenks Sara7,Templeton Kate7ORCID, ,Dold Christina8ORCID,Lambe Teresa8ORCID,Pollard Andrew8,Mentzer Alexander J9ORCID,Knight Julian C9ORCID, ,Dunachie Susanna10111213ORCID,Klenerman Paul101214,Barnes Eleanor101214,Carson Alan2ORCID,McWhirter Laura2ORCID,Hussell Tracy4ORCID,Fragkoudis Rennos6ORCID,Rosser Susan5ORCID,Cavanagh David3ORCID,Cowan Graeme3,Menon Madhvi4ORCID,Marsh Joseph A1ORCID,Kleinjan Dirk A5ORCID,Gilbert Nick1ORCID

Affiliation:

1. MRC Human Genetics Unit, Institute of Genetics and Cancer, University of Edinburgh; Western General Hospital

2. Centre for Clinical Brain Sciences, University of Edinburgh

3. Institute of Immunology and Infection Research, School of Biological Sciences, University of Edinburgh

4. Division of Infection, Immunity & Respiratory Medicine, School of Biological Sciences, University of Manchester; Oxford Rd

5. Centre for Synthetic and Systems Biology, School of Biological Sciences, University of Edinburgh

6. Edinburgh Genome Foundry, University of Edinburgh

7. Department of Clinical Biochemistry, Royal Infirmary of Edinburgh

8. Oxford Vaccine Group, Centre for Clinical Vaccinology and Tropical Medicine, University of Oxford

9. Wellcome Centre for Human Genetics, Nuffield Department of Medicine, University of Oxford

10. Peter Medawar Building for Pathogen Research, Nuffield Dept. of Clinical Medicine, University of Oxford

11. NDM Centre for Global Health Research, Nuffield Dept. of Clinical Medicine, University of Oxford

12. NIHR Oxford Biomedical Research Centre, Oxford University Hospitals NHS Foundation Trust

13. Mahidol-Oxford Tropical Medicine Research Unit

14. Translational Gastroenterology Unit, University of Oxford

Abstract

Even within a single protein, antibody binding can have beneficial, neutral, or harmful effects during the response to infection. Resolving a polyclonal antibody repertoire across a pathogen’s proteome to specific epitopes may therefore explain much of the heterogeneity in susceptibility to infectious disease. However, the three-dimensional nature of antibody-epitope interactions makes the discovery of non-obvious targets challenging. We implemented a novel computational method and synthetic biology pipeline for identifying epitopes that are functionally important in the SARS-CoV-2 proteome and identified an IgM-dominant response to an exposed Membrane protein epitope which to our knowledge is the strongest correlate of severe disease identified to date (adjusted OR 72.14, 95% CI: 9.71 – 1300.15), stronger even than the exponential association of severe disease with age. We also identify persistence (> 2 years) of this IgM response in individuals with longCOVID, and a correlation with fatigue and depression symptom burden. The repetitive arrangement of this epitope and the pattern of isotype class switching is consistent with this being a previously unrecognized T independent antigen. These findings point to a coronavirus host-pathogen interaction characteristic of severe virus driven immune pathology. This epitope is a promising vaccine and therapeutic target as it is highly conserved through SARS-CoV-2 variant evolution in humans to date and in related coronaviruses (e.g. SARS-CoV), showing far less evolutionary plasticity than targets on the Spike protein. This provides a promising biomarker for longCOVID and a target to complement Spike-directed vaccination which could broaden humoral protection from severe or persistent disease or novel coronavirus spillovers.

Publisher

eLife Sciences Publications, Ltd

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