Heritability of the melatonin synthesis variability in autism spectrum disorders

被引:0
作者
Marion Benabou
Thomas Rolland
Claire S. Leblond
Gaël A. Millot
Guillaume Huguet
Richard Delorme
Marion Leboyer
Cécile Pagan
Jacques Callebert
Erik Maronde
Thomas Bourgeron
机构
[1] Institut Pasteur,Human Genetics and Cognitive Functions Unit
[2] Genes,CNRS UMR3571
[3] Synapses and Cognition,Bioinformatics and biostatistics HUB
[4] Institut Pasteur,Psychiatry Department
[5] Paris Descartes University,INSERM U955
[6] Paris Diderot University,Service de Biochimie et Biologie Moléculaire
[7] C3BI,Institute for Cellular and Molecular Anatomy
[8] USR 3756 IP CNRS,undefined
[9] Institut Pasteur,undefined
[10] Child and Adolescent Psychiatry Department,undefined
[11] Hôpital Robert Debré,undefined
[12] Fondation Fondamental,undefined
[13] Hôpital Henri Mondor-Albert Chenevier,undefined
[14] AP-HP,undefined
[15] Université Paris Est,undefined
[16] Translational Psychiatry,undefined
[17] Paris-Est University,undefined
[18] INSERM U942,undefined
[19] Hôpital Lariboisière,undefined
[20] Dr. Senckenbergische Anatomie,undefined
[21] Goethe-University,undefined
来源
Scientific Reports | / 7卷
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摘要
Autism Spectrum Disorders (ASD) are heterogeneous neurodevelopmental disorders with a complex genetic architecture. They are characterized by impaired social communication, stereotyped behaviors and restricted interests and are frequently associated with comorbidities such as intellectual disability, epilepsy and severe sleep disorders. Hyperserotonemia and low melatonin levels are among the most replicated endophenotypes reported in ASD, but their genetic causes remain largely unknown. Based on the biochemical profile of 717 individuals including 213 children with ASD, 128 unaffected siblings and 376 parents and other relatives, we estimated the heritability of whole-blood serotonin, platelet N-acetylserotonin (NAS) and plasma melatonin levels, as well as the two enzymes arylalkylamine N-acetyltransferase (AANAT) and acetylserotonin O-methyltransferase (ASMT) activities measured in platelets. Overall, heritability was higher for NAS (0.72 ± 0.091) and ASMT (0.59 ± 0.097) compared with serotonin (0.31 ± 0.078), AANAT (0.34 ± 0.077) and melatonin (0.22 ± 0.071). Bivariate analyses showed high phenotypic and genetic correlations between traits of the second step of the metabolic pathway (NAS, ASMT and melatonin) indicating the contribution of shared genetic factors. A better knowledge of the heritability of the melatonin synthesis variability constitutes an important step to identify the factors that perturb this pathway in individuals with ASD.
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