Synapsin autoantibodies during pregnancy are associated with fetal abnormalities

Anti-neuronal autoantibodies can be transplacentally transferred during pregnancy and may cause detrimental effects on fetal development. It is unclear whether autoantibodies against synapsin-I, one of the most abundant synaptic proteins, are associated with developmental abnormalities in humans. We...

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Autores principales: Bünger, Isabel, Talucci, Ivan, Kreye, Jakob, Höltje, Markus, Makridis, Konstantin L., Foverskov Rasmussen, Helle, van Hoof, Scott, Cordero-Gomez, César, Ullrich, Tim, Sedlin, Eva, Kreissner, Kai Oliver, Hoffmann, Christian, Milovanovic, Dragomir, Turko, Paul, Paul, Friedemann, Meckies, Jessica, Verlohren, Stefan, Henrich, Wolfgang, Chaoui, Rabih, Maric, Hans Michael, Kaindl, Angela M., Prüss, Harald
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2023
Materias:
Full Length Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10483408/
https://www.ncbi.nlm.nih.gov/pubmed/37692096
http://dx.doi.org/10.1016/j.bbih.2023.100678
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author Bünger, Isabel
Talucci, Ivan
Kreye, Jakob
Höltje, Markus
Makridis, Konstantin L.
Foverskov Rasmussen, Helle
van Hoof, Scott
Cordero-Gomez, César
Ullrich, Tim
Sedlin, Eva
Kreissner, Kai Oliver
Hoffmann, Christian
Milovanovic, Dragomir
Turko, Paul
Paul, Friedemann
Meckies, Jessica
Verlohren, Stefan
Henrich, Wolfgang
Chaoui, Rabih
Maric, Hans Michael
Kaindl, Angela M.
Prüss, Harald
author_facet Bünger, Isabel
Talucci, Ivan
Kreye, Jakob
Höltje, Markus
Makridis, Konstantin L.
Foverskov Rasmussen, Helle
van Hoof, Scott
Cordero-Gomez, César
Ullrich, Tim
Sedlin, Eva
Kreissner, Kai Oliver
Hoffmann, Christian
Milovanovic, Dragomir
Turko, Paul
Paul, Friedemann
Meckies, Jessica
Verlohren, Stefan
Henrich, Wolfgang
Chaoui, Rabih
Maric, Hans Michael
Kaindl, Angela M.
Prüss, Harald
author_sort Bünger, Isabel
collection PubMed
description Anti-neuronal autoantibodies can be transplacentally transferred during pregnancy and may cause detrimental effects on fetal development. It is unclear whether autoantibodies against synapsin-I, one of the most abundant synaptic proteins, are associated with developmental abnormalities in humans. We recruited a cohort of 263 pregnant women and detected serum synapsin-I IgG autoantibodies in 13.3% using cell-based assays. Seropositivity was strongly associated with abnormalities of fetal development including structural defects, intrauterine growth retardation, amniotic fluid disorders and neuropsychiatric developmental diseases in previous children (odds ratios of 3–6.5). Autoantibodies reached the fetal circulation and were mainly of IgG1/IgG3 subclasses. They bound to conformational and linear synapsin-I epitopes, five distinct epitopes were identified using peptide microarrays. The findings indicate that synapsin-I autoantibodies may be clinically useful biomarkers or even directly participate in the disease process of neurodevelopmental disorders, thus being potentially amenable to antibody-targeting interventional strategies in the future.
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spelling pubmed-104834082023-09-08 Synapsin autoantibodies during pregnancy are associated with fetal abnormalities Bünger, Isabel Talucci, Ivan Kreye, Jakob Höltje, Markus Makridis, Konstantin L. Foverskov Rasmussen, Helle van Hoof, Scott Cordero-Gomez, César Ullrich, Tim Sedlin, Eva Kreissner, Kai Oliver Hoffmann, Christian Milovanovic, Dragomir Turko, Paul Paul, Friedemann Meckies, Jessica Verlohren, Stefan Henrich, Wolfgang Chaoui, Rabih Maric, Hans Michael Kaindl, Angela M. Prüss, Harald Brain Behav Immun Health Full Length Article Anti-neuronal autoantibodies can be transplacentally transferred during pregnancy and may cause detrimental effects on fetal development. It is unclear whether autoantibodies against synapsin-I, one of the most abundant synaptic proteins, are associated with developmental abnormalities in humans. We recruited a cohort of 263 pregnant women and detected serum synapsin-I IgG autoantibodies in 13.3% using cell-based assays. Seropositivity was strongly associated with abnormalities of fetal development including structural defects, intrauterine growth retardation, amniotic fluid disorders and neuropsychiatric developmental diseases in previous children (odds ratios of 3–6.5). Autoantibodies reached the fetal circulation and were mainly of IgG1/IgG3 subclasses. They bound to conformational and linear synapsin-I epitopes, five distinct epitopes were identified using peptide microarrays. The findings indicate that synapsin-I autoantibodies may be clinically useful biomarkers or even directly participate in the disease process of neurodevelopmental disorders, thus being potentially amenable to antibody-targeting interventional strategies in the future. Elsevier 2023-08-29 /pmc/articles/PMC10483408/ /pubmed/37692096 http://dx.doi.org/10.1016/j.bbih.2023.100678 Text en © 2023 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Full Length Article
Bünger, Isabel
Talucci, Ivan
Kreye, Jakob
Höltje, Markus
Makridis, Konstantin L.
Foverskov Rasmussen, Helle
van Hoof, Scott
Cordero-Gomez, César
Ullrich, Tim
Sedlin, Eva
Kreissner, Kai Oliver
Hoffmann, Christian
Milovanovic, Dragomir
Turko, Paul
Paul, Friedemann
Meckies, Jessica
Verlohren, Stefan
Henrich, Wolfgang
Chaoui, Rabih
Maric, Hans Michael
Kaindl, Angela M.
Prüss, Harald
Synapsin autoantibodies during pregnancy are associated with fetal abnormalities
title Synapsin autoantibodies during pregnancy are associated with fetal abnormalities
title_full Synapsin autoantibodies during pregnancy are associated with fetal abnormalities
title_fullStr Synapsin autoantibodies during pregnancy are associated with fetal abnormalities
title_full_unstemmed Synapsin autoantibodies during pregnancy are associated with fetal abnormalities
title_short Synapsin autoantibodies during pregnancy are associated with fetal abnormalities
title_sort synapsin autoantibodies during pregnancy are associated with fetal abnormalities
topic Full Length Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10483408/
https://www.ncbi.nlm.nih.gov/pubmed/37692096
http://dx.doi.org/10.1016/j.bbih.2023.100678
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