A preliminary study of lamotrigine for the treatment of posttraumatic stress disorder

Hertzberg, Michael A; Butterfield, Marian I; Feldman, Michelle E; Beckham, Jean C; Sutherland, Suzanne M; Connor, Kathryn M; Davidson, Jonathan R.T

« Previous Next »Biological Psychiatry
Volume 45, Issue 9 , Pages 1226-1229, May 1999

A preliminary study of lamotrigine for the treatment of posttraumatic stress disorder

Michael A Hertzberg
- Duke University Medical Center, Department of Psychiatry, Durham, NC, USA (MAH, MIB, JCB, SMS, KMC, JRTD)
- Durham Veterans Affairs Medical Center, Durham, NC, USA (MAH, MIB, MEF, JCB)
- Address reprint requests to Michael A. Hertzberg, MD, Durham VAMC, 116A, 508 Fulton Street, Durham, NC 27705
Marian I Butterfield
- Duke University Medical Center, Department of Psychiatry, Durham, NC, USA (MAH, MIB, JCB, SMS, KMC, JRTD)
- Durham Veterans Affairs Medical Center, Durham, NC, USA (MAH, MIB, MEF, JCB)
Michelle E Feldman
- Durham Veterans Affairs Medical Center, Durham, NC, USA (MAH, MIB, MEF, JCB)
Jean C Beckham
- Duke University Medical Center, Department of Psychiatry, Durham, NC, USA (MAH, MIB, JCB, SMS, KMC, JRTD)
- Durham Veterans Affairs Medical Center, Durham, NC, USA (MAH, MIB, MEF, JCB)
Suzanne M Sutherland
- Duke University Medical Center, Department of Psychiatry, Durham, NC, USA (MAH, MIB, JCB, SMS, KMC, JRTD)
Kathryn M Connor
- Duke University Medical Center, Department of Psychiatry, Durham, NC, USA (MAH, MIB, JCB, SMS, KMC, JRTD)
Jonathan R.T Davidson
- Duke University Medical Center, Department of Psychiatry, Durham, NC, USA (MAH, MIB, JCB, SMS, KMC, JRTD)

Received 4 August 1998; received in revised form 7 December 1998; accepted 10 December 1998.

Abstract

Background: The anticonvulsant, lamotrigine, may be useful for symptom management in PTSD.

Methods: Subjects enrolled in a 12-week double-blind evaluation of lamotrigine and placebo. Patients were randomized 2:1 to either lamotrigine or placebo. Lamotrigine was initiated at 25 mg/day and slowly titrated every 1 to 2 weeks over 8 weeks to a maximum dosage of 500 mg/day if tolerated.

Results: Fifteen subjects entered treatment, fourteen of whom returned for subsequent visits. Of 10 patients who received lamotrigine, 5 (50%) responded according to the DGRP, compared to 1 of 4 (25%) who received placebo. Lamotrigine patients showed improvement on reexperiencing and avoidance/numbing symptoms compared to placebo patients. Treatments were generally well tolerated.

Conclusions: Lamotrigine may be effective as a primary psychopharmacologic treatment in both combat and civilian PTSD and could also be considered as an adjunct to antidepressant therapy used in the treatment of PTSD. These promising results warrant further large sample double-blind, placebo-controlled trials.

Keywords: PTSD, lamotrigine, anticonvulsant, psychopharmacology, kindling