Quantitative Susceptibility Mapping MRI in Deep-Brain Nuclei in First-Episode Psychosis

Overview

Journal Schizophr Bull

Publisher Oxford University Press

Specialty Psychiatry

Date 2023 Apr 8

PMID 37030007

Authors

Marisleydis Garcia Saborit

Alejandro Jara

Nestor Munoz

Carlos Milovic

Angeles Tepper

Luz Maria Alliende

Carlos Mena

Barbara Iruretagoyena

Juan Pablo Ramirez-Mahaluf

Camila Diaz

Ruben Nachar

Carmen Paz Castaneda

Alfonso Gonzalez

Juan Undurraga

Nicolas Crossley

Cristian Tejos

Affiliations

Soon will be listed here.

Abstract

Background: Psychosis is related to neurochemical changes in deep-brain nuclei, particularly suggesting dopamine dysfunctions. We used an magnetic resonance imaging-based technique called quantitative susceptibility mapping (QSM) to study these regions in psychosis. QSM quantifies magnetic susceptibility in the brain, which is associated with iron concentrations. Since iron is a cofactor in dopamine pathways and co-localizes with inhibitory neurons, differences in QSM could reflect changes in these processes.

Methods: We scanned 83 patients with first-episode psychosis and 64 healthy subjects. We reassessed 22 patients and 21 control subjects after 3 months. Mean susceptibility was measured in 6 deep-brain nuclei. Using linear mixed models, we analyzed the effect of case-control differences, region, age, gender, volume, framewise displacement (FD), treatment duration, dose, laterality, session, and psychotic symptoms on QSM.

Results: Patients showed a significant susceptibility reduction in the putamen and globus pallidus externa (GPe). Patients also showed a significant R2* reduction in GPe. Age, gender, FD, session, group, and region are significant predictor variables for QSM. Dose, treatment duration, and volume were not predictor variables of QSM.

Conclusions: Reduction in QSM and R2* suggests a decreased iron concentration in the GPe of patients. Susceptibility reduction in putamen cannot be associated with iron changes. Since changes observed in putamen and GPe were not associated with symptoms, dose, and treatment duration, we hypothesize that susceptibility may be a trait marker rather than a state marker, but this must be verified with long-term studies.

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