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Suicide Risk in Veterans Health Administration Patients with Mental Health Diagnoses Initiating Lithium or Valproate: a Historical Prospective Cohort Study

Overview
Journal BMC Psychiatry
Publisher Biomed Central
Specialty Psychiatry
Date 2014 Dec 18
PMID 25515091
Citations 4
Authors
Affiliations
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Abstract

Background: Lithium has been reported in some, but not all, studies to be associated with reduced risks of suicide death or suicidal behavior. The objective of this nonrandomized cohort study was to examine whether lithium was associated with reduced risk of suicide death in comparison to the commonly-used alternative treatment, valproate.

Methods: A propensity score-matched cohort study was conducted of Veterans Health Administration patients (n=21,194/treatment) initiating lithium or valproate from 1999-2008.

Results: Matching produced lithium and valproate treatment groups that were highly similar in all 934 propensity score covariates, including indicators of recent suicidal behavior, but recent suicidal ideation was not able to be included. In the few individuals with recently diagnosed suicidal ideation, a significant imbalance existed with suicidal ideation more prevalent at baseline among individuals initiating lithium than valproate (odds ratio (OR) 1.30, 95% CI 1.09, 1.54; p=0.003). No significant differences in suicide death were observed over 0-365 days in A) the primary intent-to-treat analysis (lithium/valproate conditional odds ratio (cOR) 1.22, 95% CI 0.82, 1.81; p=0.32); B) during receipt of initial lithium or valproate treatment (cOR 0.86, 95% CI 0.46, 1.61; p=0.63); or C) after such treatment had been discontinued/modified (OR 1.51, 95% CI 0.91, 2.50; p=0.11). Significantly increased risks of suicide death were observed after the discontinuation/modification of lithium, compared to valproate, treatment over the first 180 days (OR 2.72, 95% CI 1.21, 6.11; p=0.015).

Conclusions: In this somewhat distinct sample (a predominantly male Veteran sample with a broad range of psychiatric diagnoses), no significant differences in associations with suicide death were observed between lithium and valproate treatment over 365 days. The only significant difference was observed over 0-180 days: an increased risk of suicide death, among individuals discontinuing or modifying lithium, compared to valproate, treatment. This difference could reflect risks either related to lithium discontinuation or higher baseline risks among lithium recipients (i.e., confounding) that became more evident when treatment stopped. Our findings therefore support educating patients and providers about possible suicide-related risks of discontinuing lithium even shortly after treatment initiation, and the close monitoring of patients after lithium discontinuation, if feasible. If our findings include residual confounding biasing against lithium, however, as suggested by the differences observed in diagnosed suicidal ideation, then the degree of beneficial reduction in suicide death risk associated with active lithium treatment would be underestimated. Further research is urgently needed, given the lack of interventions against suicide and the uncertainties concerning the degree to which lithium may reduce suicide risk during active treatment, increase risk upon discontinuation, or both.

Citing Articles

Impact of Lithium on Suicidality in the Veteran Population.

Stark K, Basit S, Mitchell B Fed Pract. 2022; 39(3):130-135.

PMID: 35444394 PMC: 9014926. DOI: 10.12788/fp.0241.


Effects of somatic treatments on suicidal ideation and completed suicides.

Hawkins E, Coryell W, Leung S, Parikh S, Weston C, Nestadt P Brain Behav. 2021; 11(11):e2381.

PMID: 34661999 PMC: 8613439. DOI: 10.1002/brb3.2381.


Animal models to improve our understanding and treatment of suicidal behavior.

Gould T, Georgiou P, Brenner L, Brundin L, Can A, Courtet P Transl Psychiatry. 2017; 7(4):e1092.

PMID: 28398339 PMC: 5416692. DOI: 10.1038/tp.2017.50.


Suicidal Behavior in Mood Disorders: Response to Pharmacological Treatment.

Tondo L, Baldessarini R Curr Psychiatry Rep. 2016; 18(9):88.

PMID: 27542851 DOI: 10.1007/s11920-016-0715-0.

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