AI Article Synopsis
- - Patients with sodium channel mutations experience various symptoms, such as seizures, developmental delays, and motor issues.
- - A study by Atkin et al. identified 90 compounds that reduced sodium influx in cells with a specific mutation, with amitriptyline, carvedilol, and nilvadipine being the most effective.
- - In further tests on mice, amitriptyline and fenfluramine showed strong seizure protection, but only carvedilol significantly helped mice with the specific mutation, suggesting it may be a promising treatment option.
Article Abstract
Patients with mutations that alter the function of the sodium channel present with a range of clinical features, including mild to severe seizures, developmental delay, intellectual disability, autism, feeding dysfunction, motor impairment, and hypotonia. In an effort to identify compounds that could be potentially beneficial in associated epilepsy, Atkin et al. conducted an screen which resulted in the identification of 90 compounds that effectively reduced sodium influx into the cells expressing the human R1872Q mutation. The top compounds that emerged from this screen included amitriptyline, carvedilol, and nilvadipine. In the current study, we evaluated the ability of these three compounds to increase resistance to 6 Hz or pentylenetetrazole (PTZ)-induced seizures in wild-type CF1 mice and in a mouse line expressing the human R1620L mutation. We also evaluated the effects of fenfluramine administration, which was recently associated with a 60%-90% decrease in seizure frequency in three patients with -associated epilepsy. While amitriptyline, carvedilol, and fenfluramine provided robust protection against induced seizures in CF1 mice, only carvedilol was able to significantly increase resistance to 6 Hz- and PTZ-induced seizures in RL/+ mutants. These results provide support for further evaluation of carvedilol as a potential treatment for patients with mutations.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11184058 | PMC |
| http://dx.doi.org/10.3389/fphar.2024.1397225 | DOI Listing |
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