Data sources

The systematic review was conducted in line with the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines [Reference Page, McKenzie, Bossuyt, Boutron, Hoffmann and Mulrow30]. The PRISMA checklist is presented in Supplementary Table S1. The protocol for the systematic review was registered on PROSPERO, the National Institute of Health Research Database (Registration Number: CRD42023438350).

A manual systematic electronic search of studies utilizing omega-3 PUFAs in psychotic disorders was conducted through the following databases: Medline, Embase, and Cochrane Central Register of Controlled Trials (CENTRAL). The search included all relevant articles published until November 2024, without language restrictions. The following subject heading keywords were used to find all relevant articles: psychosis OR psychotic disorder(s) OR schizophrenia OR schizophrenia spectrum OR non-affective disorder(s) OR FEP OR UHR for psychosis OR at-risk mental state (ARMS) AND omega-3 (n-3/ω-3) fatty acids OR essential fatty acids (EFAs) OR PUFAs OR EPA OR DHA OR fish oil OR nutritional supplement. A manual search was further performed for the above references from the papers identified, relevant reviews, Trials Central (http://www.trialscentral.org), the ISRCTN (http://controlled-trials.com), and Clinical Trials (http://clinicaltrials.gov) registries.

Study selection

Double-blind placebo-controlled studies examining the therapeutic effect of omega-3 PUFAs on psychotic symptoms either as a monotherapy or adjunctive therapy in adults and children with psychosis (UHR for psychosis, FEP, or established schizophrenia) either as a primary or secondary outcome were included. Unblinded, single-blind, open-label, and pilot studies were excluded. Studies examining the effect of omega-3 PUFAs on various neurochemical, biochemical, and biological compounds were excluded. Substance and/or medication-induced psychotic disorders and disorders where psychotic symptoms were a consequence of a mood disorder (i.e. affective psychotic disorders: bipolar disorder, major depressive disorder) were additionally excluded. A diagnosis of a psychotic illness required the utilization of operational criteria including the Diagnostic and Statistical Manual of Mental Disorders (DSM) – IV [31] or the International Classification of Disease (ICD) – 10 [32] for FEP and schizophrenia, or the Comprehensive Assessment of At-Risk Mental States (CAARMS) [Reference Yung, Yuen, McGorry, Phillips, Kelly and Dell’Olio33], or Structured Interview for Psychosis Risk Syndromes (SIPS) [Reference Miller, McGlashan, Rosen, Cadenhead, Cannon and Ventura34], for individuals with UHR for psychosis. For all studies, symptomatic assessment was either considered a primary or secondary outcome measure.

Data extraction

Two reviewers (A.R., B.H.) independently assessed and extracted relevant data including participants’ age, diagnosis, and type of antipsychotic treatment, trial duration, baseline psychometric scores and/or difference in scores between baseline and follow-up review(s) along with type, dosage, and prescription schedule of intervention. Corresponding authors of eligible studies were contacted by email in the event of incomplete or partly unavailable results. The following data were extracted by reviewers from July 8, 2023, and manually entered into a Microsoft Excel worksheet, later adapted into a table to visually display the results of individual studies (Table 1). Our primary analysis selected the following hierarchy of psychometric instruments: the Positive and Negative Syndrome Scale (PANSS; n = 21), the Brief Psychiatric Rating Scale (BPRS; n = 3), and the CAARMS (n = 1).

Table 1. Characteristics of randomized placebo-controlled trials of omega-3 polyunsaturated fatty acids on symptom severity of psychosis in UHR population and schizophrenia patients.

Abbreviations: BPRS, brief psychiatric rating scale; CAARMS, comprehensive assessment of at-risk mental state; CBCM, cognitive behavioural case management; DHA, docosahexaenoic acid; EPA, eicosapentaenoic acid; N/A indicates data not applicable; PANSS, positive and negative syndrome scale. - indicates data unavailable; SD, standard deviation.

^a Efficacy of omega-3 treatment on symptom improvement for each individual study. T = PANSS total scores; P = PANSS positive subscale; N = PANSS negative subscale; s = significant improvement of symptoms; sdc = significant decline of symptoms; ns = no significant change of symptoms.

^b Medium-term/long-term follow-up outcome study from a previous randomized placebo-controlled trial.

^c Vitamin E was treated as an active comparison in the study.

^d Two different studies were published in a single article.

^e Patients received daily dosages of 2 g EPA, 1 g DHA, and 0.3 g alpha-lipoic acid.

^f Mean time to follow-up with a range of 1.5–5.7 years.

^g Mean age of participants.

^h Intervention groups included minocycline, omega-3, combined minocycline, and omega-3 or double placebo. Data presented are for omega-3 and double placebo only.

Statistical analysis

Mean change in psychometric data was calculated by subtracting post-intervention scores with baseline scores while SD change from baseline was calculated using the following equation: $ {\mathrm{SD}}_{\mathrm{Change}}=\sqrt{\left({\mathrm{SD}}_{\mathrm{B}\mathrm{aseline}}^2+{\mathrm{SD}}_{\mathrm{Final}}^2-2{\rho}_{\mathrm{B},\mathrm{F}}{\mathrm{SD}}_{\mathrm{B}\mathrm{aseline}}{\mathrm{SD}}_{\mathrm{Final}}\right)} $ . Correlation coefficient was estimated at 0.5 in the case of an unknown value. Results of mean difference were presented as negative values representing a reduction in psychotic symptoms.

The Cochrane Review Manager version 5.4 was used to evaluate any treatment effect between the omega-3 and control groups. The effect sizes and covariate effects were combined across studies using random-effects meta-analysis models with inverse variance weighting used to summarize the effects across studies and estimate the SMDs and their corresponding 95% confidence intervals (CIs) for continuous outcomes. Finally, the heterogeneity of studies was assessed using the I ² statistic before evaluating any publication bias using a funnel plot asymmetry.