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Review of pharmacogenetics of antiseizure medications: focusing on genetic variants of mechanistic targets

  • Chih Hsiang Lin
  • , Chen Jui Ho
  • , Shih Ying Chen
  • , Yan Ting Lu
  • , Meng Han Tsai*
  • *Corresponding author for this work
  • Chang Gung University

Research output: Contribution to journalReview articlepeer-review

3 Scopus citations

Abstract

Antiseizure medications (ASMs) play a central role in seizure management, however, unpredictability in the response to treatment persists, even among patients with similar seizure manifestations and clinical backgrounds. An objective biomarker capable of reliably predicting the response to ASMs would profoundly impact epilepsy treatment. Presently, clinicians rely on a trial-and-error approach when selecting ASMs, a time-consuming process that can result in delays in receiving alternative non-pharmacological therapies such as a ketogenetic diet, epilepsy surgery, and neuromodulation therapies. Pharmacogenetic studies investigating the correlation between ASMs and genetic variants regarding their mechanistic targets offer promise in predicting the response to treatment. Sodium channel subunit genes have been extensively studied along with other ion channels and receptors as targets, however, the results have been conflicting, possibly due to methodological disparities including inconsistent definitions of drug response, variations in ASM combinations, and diversity of genetic variants/genes studied. Nonetheless, these studies underscore the potential effect of genetic variants on the mechanism of ASMs and consequently the prediction of treatment response. Recent advances in sequencing technology have led to the generation of large genetic datasets, which may be able to enhance the predictive accuracy of the response to ASMs.

Original languageEnglish
Article number1411487
Pages (from-to)1411487
JournalFrontiers in Pharmacology
Volume15
DOIs
StatePublished - 2024

Bibliographical note

Copyright © 2024 Lin, Ho, Chen, Lu and Tsai.

Keywords

  • antiseizure medication
  • drug-resistant epilepsy
  • genetic variants
  • mechanistic targets
  • pharmacogenetic studies

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