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Review

Ganaxolone treatment for epilepsy patients: from pharmacology to place in therapy

ORCID Icon, & ORCID Icon
Pages 1317-1332 | Received 15 Feb 2021, Accepted 15 Mar 2021, Published online: 29 Mar 2021
 

ABSTRACT

Introduction: Nonsulfated neurosteroids can provide phasic and tonic inhibition through activation of synaptic and extra-synaptic γ-aminobutyric acid (GABA)A receptors, exhibiting a greater potency for the latter. These actions occur by interacting with modulatory sites that are distinct from those bound by benzodiazepines and barbiturates. Ganaxolone (GNX) is a synthetic analog of the endogenous neurosteroid allopregnanolone and a member of a novel class of neuroactive steroids called epalons.

Areas covered: The authors review the pharmacology of GNX, summarize the main clinical evidence about its antiseizure efficacy and tolerability, and suggest implications for clinical practice and future research.

Expert opinion: The clinical development of GNX is mainly oriented to target unmet needs and focused on status epilepticus and rare genetic epilepsies that have few or no treatment options.

The availability of oral and intravenous formulations allows reaching adult and pediatric patients in acute and chronic care settings. Further evidence will complement the understanding of the potentialities of GNX and possibly lead to indications for use in clinical practice.

Article highlights

  • Nonsulfated neurosteroids can provide phasic and tonic inhibition through activation of synaptic and extra-synaptic γ-aminobutyric acid (GABA)A receptors

  • Ganaxolone (GNX) is a synthetic analog of the endogenous neurosteroid allopregnanolone

  • Ganaxolone displayed antiseizure properties in a broad range of experimental models

  • The clinical development of GNX is mainly oriented to target unmet needs and focused on status epilepticus and rare genetic epilepsies

  • The availability of oral and intravenous formulations allows reaching adult and pediatric patients in acute and chronic care settings

Declaration of interest

S Lattanzi has received speaker’s or consultancy fees from Eisai, GW Pharmaceuticals, and UCB Pharma and has served on advisory boards for Angelini Pharma, Arvelle Therapeutics, BIAL, and GW Pharmaceuticals. P Striano has received fees and research grants from GW Pharmaceuticals, Zogenix, BioMarin, and Kolfarma. The authors have no other relevant affiliations or financial involvement with any organization or entity with a financial interest in or conflict with the subject matter or materials discussed in this manuscript apart from those disclosed.

Reviewer disclosures

Peer reviewers on this manuscript have no relevant financial or other relationships to disclose.

Additional information

Funding

This paper was not funded.

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