The psychosis metabolic risk calculator (PsyMetRiC) for young people with psychosis: International external validation and site-specific recalibration in two independent European samples

Perry, Benjamin I.; Vandenberghe, Frederik; Garrido-Torres, Nathalia; Osimo, Emanuele F.; Piras, Marianna; Vázquez Bourgon, Javier; Upthegrove, Rachel; Grosu, Claire; Ortiz-García de la Foz, Víctor; Jones, Peter B.; Laaboub, Nermine; Ruiz-Veguilla, Miguel; Stochl, Jan; Dubath, Celine; Canal-Rivero, Manuel; Mallikarjun, Pavan; Reymond-Delacrétaz, Aurélie; Ansermot, Nicolas; Fernandez-Egea, Emilio; Crettol, Severine

doi:10.1016/j. lanepe.2022.100493

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PsychosisMetabolicRi ... (735.8Kb)

Identificadores

URI: https://hdl.handle.net/10902/26769

DOI: 10.1016/j. lanepe.2022.100493

ISSN: 2666-7762

Fecha

2022-08-19

Derechos

Attribution 4.0 International

Publicado en

The Lancet Regional Health - Europe 2022; 22: 100493

Editorial

Elsevier

Enlace a la publicación

https://doi.org/10.1016/j. lanepe.2022.100493

Palabras clave

Psychosis

Early Intervention

Risk Prediction Algorithm

Metabolic Syndrome

International Validation

PsyMetab

PAFIP

Resumen/Abstract

Background: Cardiometabolic dysfunction is common in young people with psychosis. Recently, the Psychosis Metabolic Risk Calculator (PsyMetRiC) was developed and externally validated in the UK, predicting up-to six-year risk of metabolic syndrome (MetS) from routinely collected data. The full-model includes age, sex, ethnicity, body-mass index, smoking status, prescription of metabolically-active antipsychotic medication, high-density lipoprotein, and triglyceride concentrations; the partial-model excludes biochemical predictors. Methods: To move toward a future internationally-useful tool, we externally validated PsyMetRiC in two independent European samples. We used data from the PsyMetab (Lausanne, Switzerland) and PAFIP (Cantabria, Spain) cohorts, including participants aged 16-35y without MetS at baseline who had 1-6y follow-up. Predictive performance was assessed primarily via discrimination (C-statistic), calibration (calibration plots), and decision curve analysis. Site-specific recalibration was considered. Findings: We included 1024 participants (PsyMetab n=558, male=62%, outcome prevalence=19%, mean follow-up=2.48y; PAFIP n=466, male=65%, outcome prevalence=14%, mean follow-up=2.59y). Discrimination was better in the full- compared with partial-model (PsyMetab=full-model C=0.73, 95% C.I., 0.68-0.79, partial-model C=0.68, 95% C.I., 0.62-0.74; PAFIP=full-model C=0.72, 95% C.I., 0.66-0.78; partial-model C=0.66, 95% C.I., 0.60-0.71). As expected, calibration plots revealed varying degrees of miscalibration, which recovered following site-specific recalibration. PsyMetRiC showed net benefit in both new cohorts, more so after recalibration. Interpretation: The study provides evidence of PsyMetRiC's generalizability in Western Europe, although further local and international validation studies are required. In future, PsyMetRiC could help clinicians internationally to identify young people with psychosis who are at higher cardiometabolic risk, so interventions can be directed effectively to reduce long-term morbidity and mortality.

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