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. 2024 Dec:89:15-23.
doi: 10.1016/j.euroneuro.2024.07.015. Epub 2024 Sep 2.

Association between exposure to antidepressants and stimulants and age at onset of mania or psychosis: A retrospective population-based cohort study

Alessandro Miola  1 Mete Ercis  2 Vanessa K Pazdernik  3 Manuel Fuentes Salgado  4 Javier Ortiz-Orendain  5 Manuel Gardea-Reséndez  6 Peggy M Gruhlke  3 Ian Michel  7 J Michael Bostwick  2 Alastair J McKean  2 Jennifer L Vande Voort  2 Aysegul Ozerdem  2 Mark A Frye  8
Affiliations

Association between exposure to antidepressants and stimulants and age at onset of mania or psychosis: A retrospective population-based cohort study

Alessandro Miola et al. Eur Neuropsychopharmacol. 2024 Dec.

Abstract

This study investigated the impact of prior antidepressant and stimulant exposure on the age at onset (AAO) of first episode mania (FEM) or psychosis (FEP). Patients with FEP and FEM born after 1985 in Olmsted County, Minnesota, were identified using the Rochester Epidemiology Project. Duration and peak dose of antidepressant and stimulant exposure were quantified by review of the electronic health record. Peak doses were converted to defined daily dose (DDD), and cumulative exposure was calculated as DDD multiplied by treatment duration. Linear models were used to assess relationships between AAO with any exposures, and cumulative antidepressant and stimulant exposures. A total of 190 FEM/FEP patients (mean AAO=20.8 ± 3.7 years) were included. There was no significant difference in AAO with vs. without exposure to antidepressants or stimulants. Cumulative antidepressant exposure correlated with a later AAO in overall sample (r = 0.28, p < 0.001), and in FEP (r = 0.33, p < 0.001). No significant correlation emerged between cumulative stimulant exposure and AAO. Multivariable modeling confirmed that cumulative antidepressant exposure (Estimate=2.42, 95 %CI=1.66-3.18, p < 0.001), but not cumulative stimulant exposure (Estimate=-0.04, 95 %CI=-1.10-1.02, p = 0.94), was associated with later AAO. Antidepressant and stimulant exposures were not associated with earlier AAO. However, cumulative antidepressant exposure was associated with later AAO. Limitations include retrospective design and relatively small sample size. Our findings may inform adolescent treatment recommendations when assessing risk for psychotropic-related adverse events. Further risk modeling investigations of antidepressants and stimulants with larger sample sizes are needed to explore the role of antidepressant and stimulant exposure in the trajectory leading to FEM/FEP.

Keywords: Age at onset; Antidepressants; Bipolar disorder; First episode; Schizophrenia; Stimulants.

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Conflict of interest statement

Declaration of competing interest JLVV has received grant-in-kind support for supplies and genotyping from Assurex Health. MAF received grant support from Assurex Health and Mayo Foundation, received CME travel and honoraria from Carnot Laboratories and American Physician Institute, and has Financial Interest/Stock ownership/Royalties from Chymia LLC. No other declaration of interests from other authors.

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