Clemizole and trazodone are effective antiseizure treatments in a zebrafish model of <scp>STXBP1</scp> disorder

Moog, Maia; Baraban, Scott C.

doi:10.1002/epi4.12604

Cited by 12 publications

(6 citation statements)

References 56 publications

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“…In this experiment, the ZebVortrack system was used to evaluate a variety of antiseizure drugs, and the results showed that these antiseizure drugs could reduce the activity frequency of larval zebra sh and suppress the seizure-like behavior induced by PTZ, which is in accordance with previous reports [34][35][36][37] .…”

Section: Discussionsupporting

confidence: 88%

Establishment of innovative ZebVortrack behavioral analysis system for quantitative epileptic seizure assessment in larval zebrafish

Chen

Cheng

Jia

et al. 2023

Preprint

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Pro-convulsant agents can cause a series of pathologic swimming behaviors in zebrafish, of which rapid “whirlpool-like” swimming is a representative seizure characteristic behavior. However, there is a lack of good and accurate method to quantify this type of swimming feature. Therefore, in this study, we attempted to establish a new larval zebrafish seizure analysis technique for quantitatively exporting the number of swirly swimming in a certain period. The MARGO software package based on MATLAB was employed to track the zebrafish swimming route and to produce the space–time coordinates. An innovative algorithm was developed based on the factors of vector angle, trajectory length, and swimming duration. Through the optimization of the algorithm, ZebVortrack, an analysis system, was established for automatically recognizing seizure-like swimming behaviors in larval zebrafish, treated with pentylenetetrazol (PTZ). Different pro-convulsant agents, and antiseizure drugs were used to evaluate the accuracy of the ZebVortrack system for larval zebrafish. In a word, we developed a new behavior-analysis system, ZebVortrack, for quantitatively identifying the swirly swimming behavior of larval zebrafish that can automatically and accurately determine the vortex numbers and seizure latency of larval zebrafish in microplate wells so as to provide a new analysis method for study of seizures and drug screening.

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Section: Discussionsupporting

confidence: 88%

Establishment of innovative ZebVortrack behavioral analysis system for quantitative epileptic seizure assessment in larval zebrafish

Chen

Cheng

Jia

et al. 2023

Preprint

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“…Another treatment option that has been considered is to trial medications that interact with serotonin receptors. The screening of various antiseizure medications in a zebrafish model of STXBP1-related disorders identified Clemizole and Trazodone as medications that decreased ictal events [64]. These findings suggest that medications with serotoninreceptor-binding affinities could be an effective antiseizure medication option, although further research is needed.…”

Section: Treatmentmentioning

confidence: 96%

“…In recent years, a zebrafish animal model for STXBP1-related disorders has been developed [69,70]. Already these models have been used to screen antiseizure medications [64] and have been used to visualize in vivo network dynamics [59]. This may function to easily screen medications, as well as monitor changes in network dynamics.…”

Section: Future Directionsmentioning

confidence: 99%

STXBP1-Related Disorders: Clinical Presentation, Molecular Function, Treatment, and Future Directions

Freibauer,

Wohlleben,

Boelman

2023

Genes

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In recent years, the affordability and availability of genetic testing have led to its increased use in clinical care. The increased frequency of testing has led to STXBP1 variants being identified as one of the more common variants associated with neurological disorders. In this review, we aim to summarize the common clinical phenotypes associated with STXBP1 pathogenic variants, provide an overview of their known natural history, and discuss current research into the genotype to phenotype correlation. We will also provide an overview of the suspected normal function of the STXBP1-encoded Munc18-1 protein, animal models, and experimental techniques that have been developed to study its function and use this information to try to explain the diverse phenotypes associated with STXBP1-related disorders. Finally, we will explore current therapies for STXBP1 disorders, including an overview of treatment goals for STXBP1-related disorders, a discussion of the current evidence for therapies, and future directions of personalized medications for STXBP1-related disorders.

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“…Recording chambers were placed on the stage of an upright microscope (Olympus BX-51W) and monitored continuously using a Zeiss Axiocam digital camera. Under visual guidance, gap-free LFP recordings (15 minute duration) were obtained from the optic tectum using a single-glass microelectrode (WPI glass #TW150 F-3) with approximately 1 µM tip diameter backfilled with 2 mM NaCl internal solution as described previously 29,[37][38][39][40] .…”

Section: Electrophysiology Assaymentioning

confidence: 99%

Testing of putative antiseizure drugs in a preclinical Dravet syndrome zebrafish model

Whyte-Fagundes,

Vance,

Carroll

et al. 2023

Preprint

Self Cite

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Dravet syndrome (DS) is a severe genetic epilepsy primarily caused byde novomutations in a voltage-activated sodium channel gene (SCN1A). Patients face life-threatening seizures that are largely resistant to available anti-seizure medications (ASM). Preclinical DS animal models are a valuable tool to identify candidate ASMs for these patients. Among these,scn1labmutant zebrafish exhibiting spontaneous seizure-like activity are particularly amenable to large-scale drug screening. Prior screening in ascn1labmutant zebrafish line generated using N-ethyl-N-nitrosourea (ENU) identified valproate, stiripentol, and fenfluramine e.g., Federal Drug Administration (FDA) approved drugs with clinical application in the DS population. Successful phenotypic screening inscn1labmutant zebrafish consists of two stages: (i) a locomotion-based assay measuring high-velocity convulsive swim behavior and (ii) an electrophysiology-based assay, usingin vivolocal field potential (LFP) recordings, to quantify electrographic seizure-like events. Using this strategy more than 3000 drug candidates have been screened inscn1labzebrafish mutants. Here, we curated a list of nine additional anti-seizure drug candidates recently identified in preclinical models: 1-EBIO, AA43279, chlorzoxazone, donepezil, lisuride, mifepristone, pargyline, soticlestat and vorinostat. First-stage locomotion-based assays inscn1labmutant zebrafish identified only 1-EBIO, chlorzoxazone and lisuride. However, second-stage LFP recording assays did not show significant suppression of spontaneous electrographic seizure activity for any of the nine anti-seizure drug candidates. Surprisingly, soticlestat induced frank electrographic seizure-like discharges in wild-type control zebrafish. Taken together, our results failed to replicate clear anti-seizure efficacy for these drug candidates highlighting a necessity for strict scientific standards in preclinical identification of ASMs.

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Clemizole and trazodone are effective antiseizure treatments in a zebrafish model of STXBP1 disorder

Cited by 12 publications

References 56 publications

Establishment of innovative ZebVortrack behavioral analysis system for quantitative epileptic seizure assessment in larval zebrafish

Establishment of innovative ZebVortrack behavioral analysis system for quantitative epileptic seizure assessment in larval zebrafish

STXBP1-Related Disorders: Clinical Presentation, Molecular Function, Treatment, and Future Directions

Testing of putative antiseizure drugs in a preclinical Dravet syndrome zebrafish model

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