Celia J. Holdsworth scite author profile

SUMMARYThe availability of animal models of epileptic seizures provides opportunities to identify novel anticonvulsants for the treatment of people with epilepsy. We found that exposure of 2-day-old zebrafish embryos to the convulsant agent pentylenetetrazole (PTZ) rapidly induces the expression of synaptic-activity-regulated genes in the CNS, and elicited vigorous episodes of calcium (Ca2+) flux in muscle cells as well as intense locomotor activity. We then screened a library of ∼2000 known bioactive small molecules and identified 46 compounds that suppressed PTZ-inducedtranscription of the synaptic-activity-regulated gene fos in 2-day-old (2 dpf) zebrafish embryos. Further analysis of a subset of these compounds, which included compounds with known and newly identified anticonvulsant properties, revealed that they exhibited concentration-dependent inhibition of both locomotor activity and PTZ-induced fos transcription, confirming their anticonvulsant characteristics. We conclude that this in situ hybridisation assay for fos transcription in the zebrafish embryonic CNS is a robust, high-throughput in vivo indicator of the neural response to convulsant treatment and lends itself well to chemical screening applications. Moreover, our results demonstrate that suppression of PTZ-induced fos expression provides a sensitive means of identifying compounds with anticonvulsant activities.

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Semicircular canal morphogenesis in the zebrafish inner ear requires the function ofgpr126(lauscher), an adhesion class G protein-coupled receptor gene

Geng

Abbas

Baxendale

et al. 2013

150

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Morphogenesis of the semicircular canal ducts in the vertebrate inner ear is a dramatic example of epithelial remodelling in the embryo, and failure of normal canal development results in vestibular dysfunction. In zebrafish and Xenopus, semicircular canal ducts develop when projections of epithelium, driven by extracellular matrix production, push into the otic vesicle and fuse to form pillars. We show that in the zebrafish, extracellular matrix gene expression is high during projection outgrowth and then rapidly downregulated after fusion. Enzymatic disruption of hyaluronan in the projections leads to their collapse and a failure to form pillars: as a result, the ears swell. We have cloned a zebrafish mutant, lauscher (lau), identified by its swollen ear phenotype. The primary defect in the ear is abnormal projection outgrowth and a failure of fusion to form the semicircular canal pillars. Otic expression of extracellular matrix components is highly disrupted: several genes fail to become downregulated and remain expressed at abnormally high levels into late larval stages. The lau mutations disrupt gpr126, an adhesion class G protein-coupled receptor gene. Expression of gpr126 is similar to that of sox10, an ear and neural crest marker, and is partially dependent on sox10 activity. Fusion of canal projections and downregulation of otic versican expression in a hypomorphic lau allele can be restored by cAMP agonists. We propose that Gpr126 acts through a cAMP-mediated pathway to control the outgrowth and adhesion of canal projections in the zebrafish ear via the regulation of extracellular matrix gene expression.

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Identification of compounds that rescue otic and myelination defects in the zebrafish adgrg6 (gpr126) mutant

Diamantopoulou

Baxendale

Léon

et al. 2019

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Adgrg6 (Gpr126) is an adhesion class G protein-coupled receptor with a conserved role in myelination of the peripheral nervous system. In the zebrafish, mutation of adgrg6 also results in defects in the inner ear: otic tissue fails to down-regulate versican gene expression and morphogenesis is disrupted. We have designed a whole-animal screen that tests for rescue of both up- and down-regulated gene expression in mutant embryos, together with analysis of weak and strong alleles. From a screen of 3120 structurally diverse compounds, we have identified 68 that reduce versican b expression in the adgrg6 mutant ear, 41 of which also restore myelin basic protein gene expression in Schwann cells of mutant embryos. Nineteen compounds unable to rescue a strong adgrg6 allele provide candidates for molecules that may interact directly with the Adgrg6 receptor. Our pipeline provides a powerful approach for identifying compounds that modulate GPCR activity, with potential impact for future drug design.

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A multiorganism pipeline for antiseizure drug discovery: Identification of chlorothymol as a novel γ‐aminobutyric acidergic anticonvulsant

et al. 2020

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Identification of compounds that rescue otic and myelination defects in the zebrafish adgrg6 (gpr126) mutant

Diamantopolou

Baxendale

Léon

et al. 2019

Preprint

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23Adgrg6 (Gpr126) is an adhesion class G protein-coupled receptor with a conserved role in 24 myelination of the peripheral nervous system. In the zebrafish, mutation of adgrg6 also 25 results in defects in the inner ear: otic tissue fails to down-regulate versican-gene expression 26 and morphogenesis is disrupted. We have designed a whole-animal screen that tests for 27 rescue of both up-and down-regulated gene expression in mutant embryos, together with 28 analysis of weak and strong alleles. From a screen of 3120 structurally diverse compounds, 29 we have identified 68 that reduce versican-b expression in the adgrg6 mutant ear, 41 of 30 which also restore myelin basic protein gene expression in Schwann cells of mutant 31 embryos. Nineteen compounds unable to rescue a strong adgrg6 allele provide candidates 32 for molecules that interact directly with the Adgrg6 receptor. Our pipeline provides a 33 powerful approach for identifying compounds that modulate GPCR activity, with potential 34 impact for future drug design. 35 36 3

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