Autism diagnosis is moving from the identification of common inherited genetic variants to a systems biology approach. The aims of the study were to explore metabolic perturbations in autism, to investigate whether the severity of autism core symptoms may be associated with specific metabolic signatures; and to examine whether the urine metabolome discriminates severe from mild-to-moderate restricted, repetitive, and stereotyped behaviors. We enrolled 57 children aged 2-11 years; thirty-one with idiopathic autism and twenty-six neurotypical (NT), matched for age and ethnicity. The urine metabolome was investigated by gas chromatography-mass spectrometry (GC-MS). The urinary metabolome of autistic children was largely distinguishable from that of NT children; food selectivity induced further significant metabolic differences. Severe autism spectrum disorder core deficits were marked by high levels of metabolites resulting from diet, gut dysbiosis, oxidative stress, tryptophan metabolism, mitochondrial dysfunction. The hierarchical clustering algorithm generated two metabolic clusters in autistic children: 85-90% of children with mild-to-moderate abnormal behaviors fell in cluster II. Our results open up new perspectives for the more general understanding of the correlation between the clinical phenotype of autistic children and their urine metabolome. Adipic acid, palmitic acid, and 3-(3-hydroxyphenyl)-3-hydroxypropanoic acid can be proposed as candidate biomarkers of autism severity.

Mussap, M., Siracusano, M., Noto, A., Fattuoni, C., Riccioni, A., Rajula, H., et al. (2020). The Urine Metabolome of Young Autistic Children Correlates with Their Clinical Profile Severity. METABOLITES, 10(11), 1-21 [10.3390/metabo10110476].

The Urine Metabolome of Young Autistic Children Correlates with Their Clinical Profile Severity

Siracusano, Martina;Curatolo, Paolo;Mazzone, Luigi
2020-11-23

Abstract

Autism diagnosis is moving from the identification of common inherited genetic variants to a systems biology approach. The aims of the study were to explore metabolic perturbations in autism, to investigate whether the severity of autism core symptoms may be associated with specific metabolic signatures; and to examine whether the urine metabolome discriminates severe from mild-to-moderate restricted, repetitive, and stereotyped behaviors. We enrolled 57 children aged 2-11 years; thirty-one with idiopathic autism and twenty-six neurotypical (NT), matched for age and ethnicity. The urine metabolome was investigated by gas chromatography-mass spectrometry (GC-MS). The urinary metabolome of autistic children was largely distinguishable from that of NT children; food selectivity induced further significant metabolic differences. Severe autism spectrum disorder core deficits were marked by high levels of metabolites resulting from diet, gut dysbiosis, oxidative stress, tryptophan metabolism, mitochondrial dysfunction. The hierarchical clustering algorithm generated two metabolic clusters in autistic children: 85-90% of children with mild-to-moderate abnormal behaviors fell in cluster II. Our results open up new perspectives for the more general understanding of the correlation between the clinical phenotype of autistic children and their urine metabolome. Adipic acid, palmitic acid, and 3-(3-hydroxyphenyl)-3-hydroxypropanoic acid can be proposed as candidate biomarkers of autism severity.
23-nov-2020
Pubblicato
Rilevanza internazionale
Articolo
Esperti anonimi
Settore MED/39 - NEUROPSICHIATRIA INFANTILE
English
Con Impact Factor ISI
autism core deficits
autism spectrum disorder
food selectivity
gut dysbiosis
hierarchical clustering analysis
metabolomics
Mussap, M., Siracusano, M., Noto, A., Fattuoni, C., Riccioni, A., Rajula, H., et al. (2020). The Urine Metabolome of Young Autistic Children Correlates with Their Clinical Profile Severity. METABOLITES, 10(11), 1-21 [10.3390/metabo10110476].
Mussap, M; Siracusano, M; Noto, A; Fattuoni, C; Riccioni, A; Rajula, Hsr; Fanos, V; Curatolo, P; Barberini, L; Mazzone, L
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2108/267729
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