Neurodevelopmental vulnerability to psychosis: developmentally-based methods enable detection of early life inhibitory control deficits that predict psychotic-like experiences at the transition to adolescence

Inhibitory control develops in early childhood, and atypical development may be a measurable marker of risk for the later development of psychosis. Additionally, inhibitory control may be a target for intervention. Behavioral performance on a developmentally appropriate Go/No-Go task including a fru...

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Bibliographic Details
Published in:Psychological medicine 2023-12, Vol.53 (16), p.7746-7755
Main Authors: Zarubin, Vanessa C., Damme, Katherine S. F., Vargas, Teresa, Osborne, K. Juston, Norton, Elizabeth S., Briggs-Gowan, Margaret, Allen, Norrina B., Wakschlag, Laurie, Mittal, Vijay A.
Format: Article
Language:English
Subjects:
Accuracy
Adolescence
Adolescent
Adolescents
Behavior
Brain research
Child
Child development
Child, Preschool
Childhood
Children
Early intervention
Electroencephalography
Electrophysiology
Event-related potentials
Frustration
Go/no-go discrimination learning
Humans
Induction
Internalization
Intervention
Life control
Long term symptoms
Longitudinal studies
Manipulation
Mental disorders
Original Article
Psychopathology
Psychosis
Psychotic Disorders - diagnosis
Response inhibition
Risk factors
Schizophrenia
Self Report
Task performance
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Summary:Inhibitory control develops in early childhood, and atypical development may be a measurable marker of risk for the later development of psychosis. Additionally, inhibitory control may be a target for intervention. Behavioral performance on a developmentally appropriate Go/No-Go task including a frustration manipulation completed by children ages 3-5 years (early childhood; = 107) was examined in relation to psychotic-like experiences (PLEs; 'tween'; ages 9-12), internalizing symptoms, and externalizing symptoms self-reported at long-term follow-up (pre-adolescence; ages 8-11). ERP N200 amplitude for a subset of these children ( = 34) with electrophysiological data during the task was examined as an index of inhibitory control. Children with lower accuracy on No-Go trials compared to Go trials in early childhood ( (1,101) = 3.976, = 0.049), evidenced higher PLEs at the transition to adolescence 4-9 years later, reflecting a specific deficit in inhibitory control. No association was observed with internalizing or externalizing symptoms. Decreased accuracy during the frustration manipulation predicted higher internalizing, (2,202) = 5.618, = 0.004, and externalizing symptoms, (2,202) = 4.663, = 0.010. Smaller N200 amplitudes were observed on No-Go trials for those with higher PLEs, (1,101) = 6.075, = 0.020; no relationship was observed for internalizing or externalizing symptoms. Long-term follow-up demonstrates for the first time a specific deficit in inhibitory control behaviorally and electrophysiology, for individuals who later report more PLEs. Decreases in task performance under frustration induction indicated risk for internalizing and externalizing symptoms. These findings suggest that pathophysiological mechanisms for psychosis are relevant and discriminable in early childhood, and further, suggest an identifiable and potentially modifiable target for early intervention.
ISSN:0033-2917
1469-8978
1469-8978
DOI:10.1017/S003329172300171X