Examining Autism Spectrum Disorders by Biomarkers: Example from the Oxytocin and Serotonin Systems

Autor/inn/en	Hammock, Elizabeth; Veenstra-VanderWeele, Jeremy; Yan, Zhongyu; Kerr, Travis M.; Morris, Marianna; Anderson, George M.; Carter, C. Sue; Cook, Edwin H.; Jacob, Suma
Titel	Examining Autism Spectrum Disorders by Biomarkers: Example from the Oxytocin and Serotonin Systems
Quelle	In: Journal of the American Academy of Child & Adolescent Psychiatry, 51 (2012) 7, S.712-721 (10 Seiten) PDF als Volltext Verfügbarkeit
Sprache	englisch
Dokumenttyp	gedruckt; online; Zeitschriftenaufsatz
ISSN	0890-8567
DOI	10.1016/j.jaac.2012.04.010
Schlagwörter	Animals; Autism; Symptoms (Individual Disorders); Brain; Behavior; Investigations; Age Differences; Correlation; Children; Adolescents; Intervention; Identification; Cognitive Development; Pervasive Developmental Disorders; Genetic Disorders + Suchen Sie Ihr Suchwort? Animal; Tier; Tiere; Autismus; Psychiatrische Symptomatik; Gehirn; Untersuchung; Age; Difference; Age difference; Altersunterschied; Korrelation; Child; Kind; Kinder; Adolescent; Adolescence; Adoleszenz; Jugend; Jugendalter; Jugendlicher; Identifikation; Identifizierung; Kognitive Entwicklung
Abstract	Objective: Autism spectrum disorder (ASD) is a heritable but highly heterogeneous neuropsychiatric syndrome, which poses challenges for research relying solely on behavioral symptoms or diagnosis. Examining biomarkers may give us ways to identify individuals who demonstrate specific developmental trajectories and etiological factors related to ASD. Plasma oxytocin (OT) and whole-blood serotonin (5-HT) levels are consistently altered in some individuals with ASD. Reciprocal relationships have been described between brain oxytocin and serotonin systems during development. We therefore investigated the relationship between these peripheral biomarkers as well as their relationships with age. Method: In our first study, we analyzed correlations between these two biomarkers in 31 children and adolescents who were diagnosed with autism and were not on medications. In our second study, we explored whether whole-blood 5-HT levels are altered in mice lacking the oxytocin receptor gene "Oxtr". Results: In humans, OT and 5-HT were negatively correlated with each other (p less than 0.05) and this relationship was most prominent in children less than 11 years old. Paralleling human findings, mice lacking "Oxtr" showed increased whole-blood 5-HT levels (p = 0.05), with this effect driven exclusively by mice less than 4 months old (p less than 0.01). Conclusions: Identifying relationships between identified ASD biomarkers may be a useful approach to connect otherwise disparate findings that span multiple systems in this heterogeneous disorder. Using neurochemical biomarkers to perform parallel studies in animal and human populations within a developmental context is a plausible approach to probe the root causes of ASD and to identify potential interventions. (Contains 1 table and 3 figures.) (As Provided).
Anmerkungen	Elsevier. 6277 Sea Harbor Drive, Orlando, FL 32887-4800. Tel: 877-839-7126; Tel: 407-345-4020; Fax: 407-363-1354; e-mail: usjcs@elsevier.com; Web site: http://www.elsevier.com
Erfasst von	ERIC (Education Resources Information Center), Washington, DC
Update	2017/4/10