PSYSCAN multi-centre study: baseline characteristics and clinical outcomes of the clinical high risk for psychosis sample

Stefania Tognin; Sandra Vieira; Dominic Oliver; Alexis E. Cullen; Mathew J. Kempton; Paolo Fusar-Poli; Andrea Mechelli; Paola Dazzan; Kate Merritt; Arija Maat; Lieuwe de Haan; Stephen M. Lawrie; Thérèse van Amelsvoort; Celso Arango; Barnaby Nelson; Silvana Galderisi; Rodrigo Bressan; Jun Soo Kwon; Romina Mizrahi; Wolfram Kawohl; Naemi Huber; Philipp Stämpfli; Achim Burrer; Anke Maatz; Matthias Kirschner; Julia Furtner-Srajer; Ana Weidenauer; Ullrich Sauerzopf; Marzena Lenczowski; Matthäus Willeit; Gabriele Sachs; Jenny Lepock; Ivana Prce; Sarah Ahmed; Margaret Maheandiran; Cory Gerritsen; Michael Kiang; Romina Mizrahi; Mark Weiser; Silvia Kyungjin Lho; Sun Young Moon; Minah Kim; Tae Young Lee; Kang Ik Kevin Cho; Graccielle Rodrigues da Cunha; Joost Janssen; Rosa Ayesa-Arriola; Erika van Hell; Rene S. Kahn

doi:10.1038/s41537-025-00598-x

PSYSCAN multi-centre study: baseline characteristics and clinical outcomes of the clinical high risk for psychosis sample

Stefania Tognin, Sandra Vieira, Dominic Oliver, Alexis E. Cullen^*, Mathew J. Kempton, Paolo Fusar-Poli, Andrea Mechelli, Paola Dazzan, Kate Merritt, Arija Maat, Lieuwe de Haan, Stephen M. Lawrie, Thérèse van Amelsvoort, Celso Arango, Barnaby Nelson, Silvana Galderisi, Rodrigo Bressan, Jun Soo Kwon, Romina Mizrahi, Wolfram KawohlNaemi Huber, Philipp Stämpfli, Achim Burrer, Anke Maatz, Matthias Kirschner, Julia Furtner-Srajer, Ana Weidenauer, Ullrich Sauerzopf, Marzena Lenczowski, Matthäus Willeit, Gabriele Sachs, Jenny Lepock, Ivana Prce, Sarah Ahmed, Margaret Maheandiran, Cory Gerritsen, Michael Kiang, Romina Mizrahi, Mark Weiser, Silvia Kyungjin Lho, Sun Young Moon, Minah Kim, Tae Young Lee, Kang Ik Kevin Cho, Graccielle Rodrigues da Cunha, Joost Janssen, Rosa Ayesa-Arriola, Erika van Hell, Rene S. Kahn,

^*Corresponding author for this work

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Abstract

Predicting outcomes in individuals at clinical high risk (CHR) of developing psychosis remains challenging using clinical metrics alone. The PSYSCAN project aimed to enhance predictive value by integrating data across clinical, environmental, neuroimaging, cognitive, and peripheral blood biomarkers. PSYSCAN employed a naturalistic, prospective design across 12 sites (Europe, Australia, Asia, Americas). Assessments were conducted at baseline, 3, 6, and 12 months, with follow-ups at 18 and 24 months to evaluate clinical and functional outcomes. The study included 238 CHR individuals and 134 healthy controls (HC). At baseline, CHR and HC groups differed significantly in age, education, IQ, and vocational and relationship status. Cannabis and tobacco use did not significantly differ between groups, however CHR individuals had higher proportion of moderate to high risk of tobacco abuse. A substantial portion of the CHR sample met DSM criteria for anxiety (53.4%) and/or mood disorders (52.9%), with some prescribed antidepressants (38.7%), antipsychotics (13.9%), or benzodiazepines (16.4%). Over the follow-up period, 25 CHR individuals (10.5%) transitioned to psychosis. However, the CHR group as a whole showed improvements in functioning and attenuated psychotic symptoms. Similar to other recent multi-centre studies, the CHR cohort exhibits high comorbidity rates and relatively low psychosis transition rates. These findings highlight the clinical heterogeneity within CHR populations and suggest that outcomes extend beyond psychosis onset, reinforcing the need for broader prognostic models that consider functional and transdiagnostic outcomes.

Original language	English
Article number	66
Journal	Schizophrenia
Volume	11
Issue number	1
DOIs	https://doi.org/10.1038/s41537-025-00598-x
Publication status	Published - 17 Apr 2025

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Tognin, S., Vieira, S., Oliver, D., Cullen, A. E., Kempton, M. J., Fusar-Poli, P., Mechelli, A., Dazzan, P., Merritt, K., Maat, A., de Haan, L., Lawrie, S. M., van Amelsvoort, T., Arango, C., Nelson, B., Galderisi, S., Bressan, R., Kwon, J. S., Mizrahi, R. (2025). PSYSCAN multi-centre study: baseline characteristics and clinical outcomes of the clinical high risk for psychosis sample. Schizophrenia, 11(1), Article 66. https://doi.org/10.1038/s41537-025-00598-x

@article{06103fb158ee456e93264c5fb50a44a8,

title = "PSYSCAN multi-centre study: baseline characteristics and clinical outcomes of the clinical high risk for psychosis sample",

abstract = "Predicting outcomes in individuals at clinical high risk (CHR) of developing psychosis remains challenging using clinical metrics alone. The PSYSCAN project aimed to enhance predictive value by integrating data across clinical, environmental, neuroimaging, cognitive, and peripheral blood biomarkers. PSYSCAN employed a naturalistic, prospective design across 12 sites (Europe, Australia, Asia, Americas). Assessments were conducted at baseline, 3, 6, and 12 months, with follow-ups at 18 and 24 months to evaluate clinical and functional outcomes. The study included 238 CHR individuals and 134 healthy controls (HC). At baseline, CHR and HC groups differed significantly in age, education, IQ, and vocational and relationship status. Cannabis and tobacco use did not significantly differ between groups, however CHR individuals had higher proportion of moderate to high risk of tobacco abuse. A substantial portion of the CHR sample met DSM criteria for anxiety (53.4%) and/or mood disorders (52.9%), with some prescribed antidepressants (38.7%), antipsychotics (13.9%), or benzodiazepines (16.4%). Over the follow-up period, 25 CHR individuals (10.5%) transitioned to psychosis. However, the CHR group as a whole showed improvements in functioning and attenuated psychotic symptoms. Similar to other recent multi-centre studies, the CHR cohort exhibits high comorbidity rates and relatively low psychosis transition rates. These findings highlight the clinical heterogeneity within CHR populations and suggest that outcomes extend beyond psychosis onset, reinforcing the need for broader prognostic models that consider functional and transdiagnostic outcomes.",

author = "Stefania Tognin and Sandra Vieira and Dominic Oliver and Cullen, {Alexis E.} and Kempton, {Mathew J.} and Paolo Fusar-Poli and Andrea Mechelli and Paola Dazzan and Kate Merritt and Arija Maat and {de Haan}, Lieuwe and Lawrie, {Stephen M.} and {van Amelsvoort}, Th{\'e}r{\`e}se and Celso Arango and Barnaby Nelson and Silvana Galderisi and Rodrigo Bressan and Kwon, {Jun Soo} and Romina Mizrahi and Wolfram Kawohl and Naemi Huber and Philipp St{\"a}mpfli and Achim Burrer and Anke Maatz and Matthias Kirschner and Julia Furtner-Srajer and Ana Weidenauer and Ullrich Sauerzopf and Marzena Lenczowski and Matth{\"a}us Willeit and Gabriele Sachs and Jenny Lepock and Ivana Prce and Sarah Ahmed and Margaret Maheandiran and Cory Gerritsen and Michael Kiang and Romina Mizrahi and Mark Weiser and Lho, {Silvia Kyungjin} and Moon, {Sun Young} and Minah Kim and Lee, {Tae Young} and Cho, {Kang Ik Kevin} and {da Cunha}, {Graccielle Rodrigues} and Joost Janssen and Rosa Ayesa-Arriola and {van Hell}, Erika and Kahn, {Rene S.}",

note = "Publisher Copyright: {\textcopyright} Crown 2025.",

year = "2025",

month = apr,

day = "17",

doi = "10.1038/s41537-025-00598-x",

language = "English",

volume = "11",

journal = "Schizophrenia",

issn = "2754-6993",

number = "1",

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Tognin, S, Vieira, S, Oliver, D, Cullen, AE, Kempton, MJ, Fusar-Poli, P, Mechelli, A, Dazzan, P, Merritt, K, Maat, A, de Haan, L, Lawrie, SM, van Amelsvoort, T, Arango, C, Nelson, B, Galderisi, S, Bressan, R, Kwon, JS, Mizrahi, R, Kawohl, W, Huber, N, Stämpfli, P, Burrer, A, Maatz, A, Kirschner, M, Furtner-Srajer, J, Weidenauer, A, Sauerzopf, U, Lenczowski, M, Willeit, M, Sachs, G, Lepock, J, Prce, I, Ahmed, S, Maheandiran, M, Gerritsen, C, Kiang, M, Mizrahi, R, Weiser, M, Lho, SK, Moon, SY, Kim, M, Lee, TY, Cho, KIK, da Cunha, GR, Janssen, J, Ayesa-Arriola, R, van Hell, E, Kahn, RS 2025, 'PSYSCAN multi-centre study: baseline characteristics and clinical outcomes of the clinical high risk for psychosis sample', Schizophrenia, vol. 11, no. 1, 66. https://doi.org/10.1038/s41537-025-00598-x

TY - JOUR

T1 - PSYSCAN multi-centre study

T2 - baseline characteristics and clinical outcomes of the clinical high risk for psychosis sample

AU - Tognin, Stefania

AU - Vieira, Sandra

AU - Oliver, Dominic

AU - Cullen, Alexis E.

AU - Kempton, Mathew J.

AU - Fusar-Poli, Paolo

AU - Mechelli, Andrea

AU - Dazzan, Paola

AU - Merritt, Kate

AU - Maat, Arija

AU - de Haan, Lieuwe

AU - Lawrie, Stephen M.

AU - van Amelsvoort, Thérèse

AU - Arango, Celso

AU - Nelson, Barnaby

AU - Galderisi, Silvana

AU - Bressan, Rodrigo

AU - Kwon, Jun Soo

AU - Mizrahi, Romina

AU - Kawohl, Wolfram

AU - Huber, Naemi

AU - Stämpfli, Philipp

AU - Burrer, Achim

AU - Maatz, Anke

AU - Kirschner, Matthias

AU - Furtner-Srajer, Julia

AU - Weidenauer, Ana

AU - Sauerzopf, Ullrich

AU - Lenczowski, Marzena

AU - Willeit, Matthäus

AU - Sachs, Gabriele

AU - Lepock, Jenny

AU - Prce, Ivana

AU - Ahmed, Sarah

AU - Maheandiran, Margaret

AU - Gerritsen, Cory

AU - Kiang, Michael

AU - Mizrahi, Romina

AU - Weiser, Mark

AU - Lho, Silvia Kyungjin

AU - Moon, Sun Young

AU - Kim, Minah

AU - Lee, Tae Young

AU - Cho, Kang Ik Kevin

AU - da Cunha, Graccielle Rodrigues

AU - Janssen, Joost

AU - Ayesa-Arriola, Rosa

AU - van Hell, Erika

AU - Kahn, Rene S.

PY - 2025/4/17

Y1 - 2025/4/17

N2 - Predicting outcomes in individuals at clinical high risk (CHR) of developing psychosis remains challenging using clinical metrics alone. The PSYSCAN project aimed to enhance predictive value by integrating data across clinical, environmental, neuroimaging, cognitive, and peripheral blood biomarkers. PSYSCAN employed a naturalistic, prospective design across 12 sites (Europe, Australia, Asia, Americas). Assessments were conducted at baseline, 3, 6, and 12 months, with follow-ups at 18 and 24 months to evaluate clinical and functional outcomes. The study included 238 CHR individuals and 134 healthy controls (HC). At baseline, CHR and HC groups differed significantly in age, education, IQ, and vocational and relationship status. Cannabis and tobacco use did not significantly differ between groups, however CHR individuals had higher proportion of moderate to high risk of tobacco abuse. A substantial portion of the CHR sample met DSM criteria for anxiety (53.4%) and/or mood disorders (52.9%), with some prescribed antidepressants (38.7%), antipsychotics (13.9%), or benzodiazepines (16.4%). Over the follow-up period, 25 CHR individuals (10.5%) transitioned to psychosis. However, the CHR group as a whole showed improvements in functioning and attenuated psychotic symptoms. Similar to other recent multi-centre studies, the CHR cohort exhibits high comorbidity rates and relatively low psychosis transition rates. These findings highlight the clinical heterogeneity within CHR populations and suggest that outcomes extend beyond psychosis onset, reinforcing the need for broader prognostic models that consider functional and transdiagnostic outcomes.

AB - Predicting outcomes in individuals at clinical high risk (CHR) of developing psychosis remains challenging using clinical metrics alone. The PSYSCAN project aimed to enhance predictive value by integrating data across clinical, environmental, neuroimaging, cognitive, and peripheral blood biomarkers. PSYSCAN employed a naturalistic, prospective design across 12 sites (Europe, Australia, Asia, Americas). Assessments were conducted at baseline, 3, 6, and 12 months, with follow-ups at 18 and 24 months to evaluate clinical and functional outcomes. The study included 238 CHR individuals and 134 healthy controls (HC). At baseline, CHR and HC groups differed significantly in age, education, IQ, and vocational and relationship status. Cannabis and tobacco use did not significantly differ between groups, however CHR individuals had higher proportion of moderate to high risk of tobacco abuse. A substantial portion of the CHR sample met DSM criteria for anxiety (53.4%) and/or mood disorders (52.9%), with some prescribed antidepressants (38.7%), antipsychotics (13.9%), or benzodiazepines (16.4%). Over the follow-up period, 25 CHR individuals (10.5%) transitioned to psychosis. However, the CHR group as a whole showed improvements in functioning and attenuated psychotic symptoms. Similar to other recent multi-centre studies, the CHR cohort exhibits high comorbidity rates and relatively low psychosis transition rates. These findings highlight the clinical heterogeneity within CHR populations and suggest that outcomes extend beyond psychosis onset, reinforcing the need for broader prognostic models that consider functional and transdiagnostic outcomes.

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U2 - 10.1038/s41537-025-00598-x

DO - 10.1038/s41537-025-00598-x

M3 - Article

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SN - 2754-6993

VL - 11

JO - Schizophrenia

JF - Schizophrenia

IS - 1

M1 - 66

ER -

PSYSCAN multi-centre study: baseline characteristics and clinical outcomes of the clinical high risk for psychosis sample

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