Prevalent and persistent new-onset autoantibodies in mild to severe COVID-19.

Prevalent and persistent new-onset autoantibodies in mild to severe COVID-19.

Publication date: Oct 17, 2024

Autoantibodies have been shown to be implied in COVID-19 but the emerging autoantibody repertoire remains largely unexplored. We investigated the new-onset autoantibody repertoire in 525 healthcare workers and hospitalized COVID-19 patients at five time points over a 16-month period in 2020 and 2021 using proteome-wide and targeted protein and peptide arrays. Our results show that prevalent new-onset autoantibodies against a wide range of antigens emerged following SARS-CoV-2 infection in relation to pre-infectious baseline samples and remained elevated for at least 12 months. We found an increased prevalence of new-onset autoantibodies after severe COVID-19 and demonstrated associations between distinct new-onset autoantibodies and neuropsychiatric symptoms post-COVID-19. Using epitope mapping, we determined the main epitopes of selected new-onset autoantibodies, validated them in independent cohorts of neuro-COVID and pre-pandemic healthy controls, and identified sequence similarities suggestive of molecular mimicry between main epitopes and the conserved fusion peptide of the SARS-CoV-2 Spike glycoprotein. Our work describes the complexity and dynamics of the autoantibody repertoire emerging with COVID-19 and supports the need for continued analysis of the new-onset autoantibody repertoire to elucidate the mechanisms of the post-COVID-19 condition.

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Concepts Keywords
Covid Adult
Healthcare Aged
Month Autoantibodies
New Autoantibodies
Pandemic COVID-19
Epitope Mapping
Epitopes
Epitopes
Female
Health Personnel
Humans
Male
Middle Aged
Molecular Mimicry
SARS-CoV-2
Spike Glycoprotein, Coronavirus
Spike Glycoprotein, Coronavirus
spike protein, SARS-CoV-2

Semantics

Type Source Name
disease MESH COVID-19
disease IDO protein
pathway REACTOME SARS-CoV-2 Infection
drug DRUGBANK Pirenzepine
disease MESH clinical significance
disease IDO cell
disease MESH cognitive dysfunction
disease MESH long COVID
disease MESH sequelae
disease MESH etiology
disease MESH inflammation
disease MESH autoimmunity
drug DRUGBANK Serine
disease IDO blood
disease MESH infection
disease IDO assay
disease MESH seroconversion
drug DRUGBANK Esomeprazole
disease MESH autoimmune diseases
drug DRUGBANK Natural alpha interferon
disease MESH joint pain
drug DRUGBANK Cholesterol
drug DRUGBANK Coenzyme M
drug DRUGBANK Zinc
drug DRUGBANK L-Tyrosine
drug DRUGBANK Albendazole
drug DRUGBANK Calcium
disease IDO host
disease MESH thyroid diseases
pathway REACTOME Translation
disease MESH viral infection
disease MESH syndromes
disease MESH infectious diseases
disease MESH anxiety
disease MESH dyspnea
disease MESH hair loss
disease MESH ageusia
disease MESH numbness
disease MESH anosmia
disease IDO symptom
disease IDO history
disease MESH Neurological manifestations
disease MESH paralysis
disease MESH confusion
disease MESH encephalopathy
drug DRUGBANK Pidolic Acid
disease IDO algorithm
drug DRUGBANK Deoxy-2-Fluoro-B-D-Cellotrioside
drug DRUGBANK Ademetionine
disease MESH depressive disorders
drug DRUGBANK Biotin
disease MESH privacy
disease MESH influenza
disease MESH pneumonia
drug DRUGBANK Ketamine
disease MESH Neuroinflammation
drug DRUGBANK Prothrombin
drug DRUGBANK Cardiolipin
disease MESH neurological disorders
disease MESH reinfection
disease MESH psychotic disorders
disease MESH systemic lupus erythematosus
pathway KEGG Systemic lupus erythematosus
disease MESH respiratory infections
disease MESH critical illness
drug DRUGBANK Thyroglobulin
drug DRUGBANK Iodine
drug DRUGBANK Ibuprofen
drug DRUGBANK Activated charcoal
drug DRUGBANK Sodium lauryl sulfate
disease IDO production
pathway REACTOME Reproduction

Original Article

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