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Novel maternal autoantibodies in autism spectrum disorder: Implications for screening and diagnosis
by
Mazón-Cabrera, Rut
, Vandormael, Patrick
, Somers, Veerle
, Brône, Bert
, Liesenborgs, Jori
in
autism spectrum disorder
/ autoantibodies
/ biomarker
/ Neuroscience
/ pregnancy
/ risk factor
2023
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Do you wish to request the book?
Novel maternal autoantibodies in autism spectrum disorder: Implications for screening and diagnosis
by
Mazón-Cabrera, Rut
, Vandormael, Patrick
, Somers, Veerle
, Brône, Bert
, Liesenborgs, Jori
in
autism spectrum disorder
/ autoantibodies
/ biomarker
/ Neuroscience
/ pregnancy
/ risk factor
2023
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Novel maternal autoantibodies in autism spectrum disorder: Implications for screening and diagnosis
Journal Article
Novel maternal autoantibodies in autism spectrum disorder: Implications for screening and diagnosis
2023
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Overview
Autism spectrum disorder (ASD) is a complex neurodevelopmental disorder for which early recognition is a major challenge. Autoantibodies against fetal brain antigens have been found in the blood of mothers of children with ASD (m-ASD) and can be transferred to the fetus where they can impact neurodevelopment by binding to fetal brain proteins. This study aims to identify novel maternal autoantibodies reactive against human fetal brain antigens, and explore their use as biomarkers for ASD screening and diagnosis.
A custom-made human fetal brain cDNA phage display library was constructed, and screened for antibody reactivity in m-ASD samples from the Simons Simplex Collection (SSC) of the Simons Foundation Autism Research Initiative (SFARI). Antibody reactivity against 6 identified antigens was determined in plasma samples of 238 m-ASD and 90 mothers with typically developing children (m-TD).
We identified antibodies to 6 novel University Hasselt (UH)-ASD antigens, including three novel m-ASD autoantigens, i.e., ribosomal protein L23 (RPL23), glyceraldehyde-3-phosphate dehydrogenase (GAPDH) and calmodulin-regulated spectrin-associated protein 3 (CAMSAP3). Antibody reactivity against a panel of four of these targets was found in 16% of m-ASD samples, compared to 4% in m-TD samples (
= 0.0049).
Maternal antibodies against 4 UH-ASD antigens could therefore provide a novel tool to support the diagnosis of ASD in a subset of individuals.
Publisher
Frontiers Media S.A
Subject
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