Genetic signatures predict social-cognitive trajectories in ultra-high-risk psychosis: a 24-month longitudinal study

Doborjeh, Z; Sumich, A; Medvedev, ON; Buchwald, K; Doborjeh, M; Singh, B; Budhraja, S; Merkin, A; Lam, M; Yee, JY; Lee, T-S; Goh, W; Lee, J; Williams, M; Lai, EM-K; Kasabov, NK

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Genetic signatures predict social-cognitive trajectories in ultra-high-risk psychosis: a 24-month longitudinal study

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Doborjeh, Z, Sumich, A ORCID: https://orcid.org/0000-0003-4333-8442, Medvedev, ON, Buchwald, K, Doborjeh, M, Singh, B, Budhraja, S, Merkin, A, Lam, M, Yee, JY, Lee, T-S, Goh, W, Lee, J, Williams, M, Lai, EM-K and Kasabov, NK, 2025. Genetic signatures predict social-cognitive trajectories in ultra-high-risk psychosis: a 24-month longitudinal study. Asian Journal of Psychiatry, 114: 104749. ISSN 1876-2018

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Official URL: https://doi.org/10.1016/j.ajp.2025.104749

Abstract

Background: Identifying biomarkers that predict social and cognitive outcomes in individuals at ultra-high risk (UHR) for psychosis remains a key challenge in preventive psychiatry. While genetic factors contribute to psychosis vulnerability, specific markers that predict individual trajectories of functional decline or resilience are still unclear.

Methods: In a 24-month longitudinal study involving UHR (n = 45) and healthy control participants (n = 54), we investigated for the first time the predictive causal relationship between key immunological genes (FABP5 family and immunoglobulins) and social-cognitive outcomes. Participants completed comprehensive assessments at baseline and four 6-month intervals. We used regression modelling and dynamic Bayesian network analysis to identify predictive relationships between gene expression and behavioral outcomes over time.

Results: FABP5 family genes (FABP5P1, FABP5P11, FABP5P9) significantly predicted verbal memory (β = 0.233, p = 0.002); working memory (β = 0.225, p = 0.004), and social skills (β =-0·190, p < 0.029), respectively, at 24 months in the UHR group. Immunoglobulin-related genes showed distinct effects: FCGR2B predicted object recognition ability (β = 0.233, p = 0.014), while GOT2 inversely predicted planning ability (β = -0.147, p = 0.067). Network analysis revealed UHR-specific temporal dependencies absent in controls, with FCGRT emerging as a central node linking genetic markers to changes in processing speed and perceptual closure.

Conclusions: This study provides the first evidence that FABP5 and immunoglobulin-related genetic markers can predict social-cognitive trajectories in individuals at risk for psychosis. These findings support the use of genetic profiling for early identification and highlight new opportunities for personalized preventive strategies in psychiatry.

Item Type:	Journal article
Publication Title:	Asian Journal of Psychiatry
Creators:	Doborjeh, Z., Sumich, A., Medvedev, O.N., Buchwald, K., Doborjeh, M., Singh, B., Budhraja, S., Merkin, A., Lam, M., Yee, J.Y., Lee, T.-S., Goh, W., Lee, J., Williams, M., Lai, E.M.-K. and Kasabov, N.K.
Publisher:	Elsevier BV
Date:	December 2025
Volume:	114
ISSN:	1876-2018
Identifiers:	Number Type 10.1016/j.ajp.2025.104749 DOI 2522825 Other
Rights:	© 2025 The Author(s). Published by Elsevier B.V. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
Divisions:	Schools > School of Social Sciences
Record created by:	Laura Borcherds
Date Added:	11 Nov 2025 11:06
Last Modified:	11 Nov 2025 11:06
URI:	https://irep.ntu.ac.uk/id/eprint/54706