Subscribe to RSS
DOI: 10.1055/s-0031-1297975
Lack of Interaction between Sertraline and Lamotrigine in Psychiatric Patients: A Retrospective Study
Publication History
received 21 September 2011
revised 16 November 2011
accepted 17 November 2011
Publication Date:
16 March 2012 (online)
Abstract
Introduction:
This study evaluates the pharmacokinetic interaction between sertraline and lamotrigine in psychiatric patients.
Methods:
We identified patients with at least 1 measurement of trough lamotrigine plasma concentration (at steady-state) during lamotrigine therapy and compared dose and plasma concentrations between patients who received lamotrigine with sertraline and patients who received lamotrigine without sertraline.
Results:
The dose corrected concentration of lamotrigine in patients receiving lamotrigine in combination with sertraline was 60.4 μmol/L×1 000/mg/day (SD: 31.1) (N=7) compared to 51.1 μmol/L×1 000/mg/day (SD: 27.6) (N=44) in patients using lamotrigine without sertraline (p=0.42).
Discussion:
The slightly slower metabolism of lamotrigine in patients receiving lamotrigine with sertraline compared with those receiving lamotrigine alone is not believed to be of clinical significance. However, due to the limited power, we may have overlooked a difference that could be clinically relevant.
-
References
- 1 Calabrese JR, Bowden CL, Sachs G et al. A placebo-controlled 18-month trial of lamotrigine and lithium maintenance treatment in recently depressed patients with bipolar I disorder. J Clin Psychiatry 2003; 64: 1013-1024
- 2 Licht RW, Nielsen JN, Gram LF et al. Lamotrigine versus lithium as maintenance treatment in bipolar I disorder: an open, randomized effectiveness study mimicking clinical practice. The 6 trial of the Danish University Antidepressant Group (DUAG-6). Bipolar Disord 2010; 12: 483-493
- 3 Dickins M, Chen C. Lamotrigine. Chemistry, Biotransformation and Pharmacokinetics. In: Levy RH, Mattson RH, Meldrum BS, Perucca E. editors. Antiepileptic Drugs. Fifth Edition ed. Philidelphia: Lippincott, Williams & Wilkins; 2002: 370-379
- 4 Rowland A, Elliot DJ, Williams JA et al. In vitro characterization of lamotrigine N2-glucuronidation and the lamotrigine-valproic acid interaction. Drug Metab Dispos 2006; 34: 1055-1062
- 5 Cipriani A, Brambilla P, Furukawa T et al. Fluoxetine versus other types of pharmacotherapy for depression. Cochrane Database Syst Rev October 2005; 19 (04) CD004185
- 6 Obach RS, Cox LM, Tremaine LM. Sertraline is metabolized by multiple cytochrome P450 enzymes, monoamine oxidases, and glucuronyl transferases in human: an in vitro study. Drug Metab Dispos 2005; 33: 262-270
- 7 GlaxoSmithKline. Lamictal prescribing information. 2007. http://us.gsk.com/products/assets/us_lamictal.pdf
- 8 Kaufman KR, Gerner R. Lamotrigine toxicity secondary to sertraline. Seizure 1998; 7: 163-165
- 9 Gidal BE, Sheth R, Parnell J et al. Evaluation of VPA dose and concentration effects on lamotrigine pharmacokinetics: implications for conversion to lamotrigine monotherapy. Epilepsy Res 2003; 57: 85-93
- 10 Reimers A, Skogvoll E, Sund JK et al. Drug interactions between lamotrigine and psychoactive drugs: evidence from a therapeutic drug monitoring service. J Clin Psychopharmacol 2005; 25: 342-348