Lamotrigine and Stevens-Johnson Syndrome Prevention

Authors

Amber N. Edinoff, Louisiana State University Health Science Center
Long H. Nguyen, Louisiana State University Health Science Center
Mary Jo Fitz-Gerald, Louisiana State University Health Science Center
Erin Crane, Louisiana State University Health Science Center
Kyle Lewis, Louisiana State University Health Science Center
Samantha St. Pierre, Louisiana State University Health Science Center
Alan David Kaye, Louisiana State University Health Science Center
Adam M. Kaye, University of the PacificFollow
Jessica S. Kaye, University of the PacificFollow
Rachel J. Kaye, Medical University of South Carolina
Sonja A. Gennuso, Louisiana State University Shreveport
Giustino Varrassi, LSU Health Sciences Center - Shreveport
Omar Viswanath, University of Arizona College of Medicine – Phoenix
Ivan Urits, Louisiana State University - Shreveport

ORCiD

Adam M. Kaye: 0000-0002-7224-3322

Document Type

Article

Publication Title

Psychopharmacology Bulletin

ISSN

2472-2448

Volume

51

Issue

2

First Page

96

Last Page

114

Publication Date

3-16-2021

Abstract

Stevens-Johnson Syndrome (SJS) is a rare life-threatening condition characterized by severe mucocutaneous epidermal necrolysis and detachment of the epidermis. The condition centers around a delayed-type hypersensitivity reaction with a complex etiology stemming from a variety of causes. The number one cause is medication-related-common ones including sulfonamides, antiepileptics, allopurinol, and nonsteroidal anti-inflammatory drugs. Genetics also play a role as several human leukocyte antigen (HLA) genotypes within certain ethnic groups have been implicated in adverse reactions to specific drugs. HLAB*15:02 has been identified in the Chinese and others of Southeast Asian origin to increase susceptibility to lamotrigine and carbamazepine-induced SJS. Furthermore, patients of Japanese origin with HLAB*31:01 and Koreans with HLA-B*44:03 are also at increased risk of SJS after receiving the same two drugs. Of the antiepileptics, one most commonly associated with SJS is lamotrigine, a pre-synaptic voltage-gated sodium channel inhibitor. Lamotrigine is an antiepileptic drug of the phenyltriazine class that is indicated for the prevention of focal and generalized seizures in epileptic patients as well as monotherapy or adjunctive maintenance treatment for Bipolar disorder. The occurrence of SJS is not a rigid contraindication to lamotrigine reintroduction in the same patient. To facilitate this, manufacturers have developed a strict re-challenge dosing regimen to facilitate successful reintroduction of lamotrigine. In order to prevent the recurrence of SJS during a re-challenge, timing of re-dose and initial rash severity must be considered. Therefore, to prevent SJS recurrence, prime lamotrigine re-challenge patients are those with mild initial rash that has not occurred within the previous 4 weeks. The Federal Food and Drug Administration recommends the testing HLA subtypes for those associated with SJS prior to starting lamotrigine.

Recommended Citation

Edinoff, A. N., Nguyen, L. H., Fitz-Gerald, M., Crane, E., Lewis, K., St. Pierre, S., Kaye, A. D., Kaye, A. M., Kaye, J. S., Kaye, R. J., Gennuso, S. A., Varrassi, G., Viswanath, O., & Urits, I. (2021). Lamotrigine and Stevens-Johnson Syndrome Prevention. Psychopharmacology Bulletin, 51(2), 96–114.
https://scholarlycommons.pacific.edu/phs-facarticles/577