Hyponatremia Secondary to Antidepressant Therapy - A Post Marketing Safety Study

Shetty, Harsha M

doi:10.4172/2329-6887.1000167

Cited by 3 publications

(1 citation statement)

References 13 publications

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“…Generalizability of results is also impacted because of limitations in the original studies. One notable example is that several cohort studies [18,[24][25][26][27][28][29][30] and case-control studies [10,23,[31][32][33] did not specify whether their patients were exposed to a single or multiple antidepressants during the study period. Our calculated effect sizes, therefore, assumed that patients only took one antidepressant during the study period, which could have translated into inflated event rates or ORs for antidepressants such as mianserin, mirtazapine, bupropion, or trazodone that are often used as add-on therapies in clinical practice.…”

Section: Strengths and Limitations Of The Studymentioning

confidence: 99%

The risk of antidepressant-induced hyponatremia: A meta-analysis of antidepressant classes and compounds

Gheysens,

Van Den Eede,

De Picker

2024

Eur. Psychiatr.

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Background. Hyponatremia (hypoNa) is a potentially serious adverse event of antidepressant treatment. Previous research suggests the risk of drug-induced hyponatremia differs between antidepressants. This meta-analysis sought to determine the risk of antidepressant-induced hypoNa, stratified by different compounds and classes. Methods. A PRISMA-compliant systematic search of Web of Science and PubMed databases was performed from inception until Jan 5, 2023, for original studies reporting incidences or risks of hypoNa in adults using antidepressants. We modelled random-effects meta-analyses to compute overall event rates and odds ratios of any and clinically relevant hypoNa for each compound and class, and ran head-to-head comparisons based on hypoNa event rates. We conducted subgroup analyses for geriatric populations and sodium cut-off value. The study is registered with PROSPERO, CRD42021269801. Results. We included 39 studies (n = 8,175,111). Exposure to antidepressants was associated with significantly increased odds of hypoNa (k = 7 studies, ). The highest event rates were found for SNRIs (7.44%), SSRIs (5.59%), and TCAs (2.66%); the lowest for mirtazapine (1.02%) and trazodone (0.89%). Compared to SSRIs, SNRIs were significantly more likely (k = 10, OR = 1.292 (1.120 -1.491), p < 0.001) and mirtazapine significantly less likely (k = 9, OR = 0.607 (0.385 -0.957), p = 0.032) to be associated with hypoNa. Conclusion.Our meta-analysis demonstrated that, while no antidepressant can be considered completely risk-free, for hypoNa-prone patients mirtazapine should be considered the treatment of choice and SNRIs should be prescribed more cautiously than SSRIs and TCAs.

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