Motor Clusters Reveal Differences in Risk for Psychosis, Cognitive Functioning, and Thalamocortical Connectivity: Evidence for Vulnerability Subtypes

Motor Clusters Reveal Differences in Risk for Psychosis, Cognitive Functioning, and Thalamocortical Connectivity: Evidence for Vulnerability Subtypes

Abnormal development of parallel cortical-striatal networks may contribute to abnormal motor, cognitive, and affective behavior prior to the onset of psychosis. Partitioning individuals at clinical high risk (CHR) using motor behavior may provide a novel perspective on different etiological pathways...

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Bibliographic Details
Published in:Clinical psychological science Vol. 6; no. 5; pp. 721 - 734
Main Authors: Dean, Derek J., Walther, Sebastian, Bernard, Jessica A., Mittal, Vijay A.
Format: Journal Article
Language:English
Published: Los Angeles, CA SAGE Publications 01-09-2018
Subjects:
movement abnormalities
cluster
vulnerability subtypes
clinical high risk
psychosis
clinical high-risk
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Summary:Abnormal development of parallel cortical-striatal networks may contribute to abnormal motor, cognitive, and affective behavior prior to the onset of psychosis. Partitioning individuals at clinical high risk (CHR) using motor behavior may provide a novel perspective on different etiological pathways or patient subtypes. A k-means cluster analysis was conducted in CHR (N = 69; 42% female, mean age = 18.67 years) young adults using theoretically distinct measures of motor behavior. The resulting subtypes were then compared on positive and negative symptoms at baseline, and 2-year risk of psychosis conversion. CHR participants were followed for 2 years to determine conversion to psychosis. CHR subtypes and healthy controls (n = 61; 57% female, mean age = 18.58 years) were compared on multiple cognitive domains and cortical-striatal connectivity. Results suggest 3 vulnerability subtypes of CHR individuals with different profiles of motor performance, symptoms, risk for conversion to psychosis, cognition, and thalamocortical connectivity. This approach may reflect a novel strategy for promoting tailored risk assessment as well as future research developing individualized medicine.
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ISSN:2167-7026
2167-7034
DOI:10.1177/2167702618773759