While the genetics of autism spectrum disorders (ASD) has been intensively studied, resulting in the identification of over 100 putative risk genes, the epigenetics of ASD has received less attention, and results have been inconsistent across studies. We aimed to investigate the contribution of DNA methylation (DNAm) to the risk of ASD and identify candidate biomarkers arising from the interaction of epigenetic mechanisms with genotype, gene expression, and cellular proportions. We performed DNAm differential analysis using whole blood samples from 75 discordant sibling pairs of the Italian Autism Network collection and estimated their cellular composition. We studied the correlation between DNAm and gene expression accounting for the potential effects of different genotypes on DNAm. We showed that the proportion of NK cells was significantly reduced in ASD siblings suggesting an imbalance in their immune system. We identified differentially methylated regions (DMRs) involved in neurogenesis and synaptic organization. Among candidate loci for ASD, we detected a DMR mapping to CLEC11A (neighboring SHANK1) where DNAm and gene expression were significantly and negatively correlated, independently from genotype effects. As reported in previous studies, we confirmed the involvement of immune functions in the pathophysiology of ASD. Notwithstanding the complexity of the disorder, suitable biomarkers such as CLEC11A and its neighbor SHANK1 can be discovered using integrative analyses even with peripheral tissues.

Perini, S., Filosi, M., Allibrio, G., Basadonne, I., Benvenuto, A., Buono, S., et al. (2023). Candidate biomarkers from the integration of methylation and gene expression in discordant autistic sibling pairs. TRANSLATIONAL PSYCHIATRY, 13(1) [10.1038/s41398-023-02407-4].

Candidate biomarkers from the integration of methylation and gene expression in discordant autistic sibling pairs

Benvenuto A.;Distefano G.;Elia M.;Malerba G.;Mazzone L.;Siracusano M.;
2023-01-01

Abstract

While the genetics of autism spectrum disorders (ASD) has been intensively studied, resulting in the identification of over 100 putative risk genes, the epigenetics of ASD has received less attention, and results have been inconsistent across studies. We aimed to investigate the contribution of DNA methylation (DNAm) to the risk of ASD and identify candidate biomarkers arising from the interaction of epigenetic mechanisms with genotype, gene expression, and cellular proportions. We performed DNAm differential analysis using whole blood samples from 75 discordant sibling pairs of the Italian Autism Network collection and estimated their cellular composition. We studied the correlation between DNAm and gene expression accounting for the potential effects of different genotypes on DNAm. We showed that the proportion of NK cells was significantly reduced in ASD siblings suggesting an imbalance in their immune system. We identified differentially methylated regions (DMRs) involved in neurogenesis and synaptic organization. Among candidate loci for ASD, we detected a DMR mapping to CLEC11A (neighboring SHANK1) where DNAm and gene expression were significantly and negatively correlated, independently from genotype effects. As reported in previous studies, we confirmed the involvement of immune functions in the pathophysiology of ASD. Notwithstanding the complexity of the disorder, suitable biomarkers such as CLEC11A and its neighbor SHANK1 can be discovered using integrative analyses even with peripheral tissues.
2023
Pubblicato
Rilevanza internazionale
Articolo
Esperti anonimi
Settore MED/39
Settore MEDS-20/B - Neuropsichiatria infantile
English
Con Impact Factor ISI
Perini, S., Filosi, M., Allibrio, G., Basadonne, I., Benvenuto, A., Buono, S., et al. (2023). Candidate biomarkers from the integration of methylation and gene expression in discordant autistic sibling pairs. TRANSLATIONAL PSYCHIATRY, 13(1) [10.1038/s41398-023-02407-4].
Perini, S; Filosi, M; Allibrio, G; Basadonne, I; Benvenuto, A; Buono, S; Bravaccio, C; Casonato, C; Ceppi, E; Curatolo, P; Bernardina, Bd; Da Ros, L; ...espandi
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/384143
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