Developmental and epileptic encephalopathies (DEE) are severe forms of early onset epilepsies, usually with genetic/metabolic aetiology, characterized by drug-resistant seizures (i.e. epileptic spasms), global developmental delay or intellectual disability and characteristic EEG pattern (i.e. hypsarrhythmia). One of the monogenic causes of DEE are expansion mutations in a GCN codon repeat of the Aristaless related homeobox (ARX) gene, which leads to a polyalanine (polyA) tract elongation. Although significant progress has been made in understanding the DEE1 pathogenesis, no efficacious drugs have been identified to stop recurrent seizures. Here we report on the epilepsy behaviour analysis of the clinical mouse model of DEE, Arx polyalanine (Arx polyAla) that express the c.330ins(GCG)7 mutation through the insertion of seven GCG alanine codons in the first polyA stretch. These mice exhibit severe spontaneous tonic-clonic seizures and present a high risk for Sudden Unexpected Death in Epilepsy (SUDEP). We present promising data on in vivo post-natal treatments with the Food-Drug Administration (FDA)-approved HDAC inhibitor Vorinostat, which anticonvulsant property has been widely reported. The treatment was done by daily intraperitoneal injection for 7 days, after quantification of baseline seizure frequency. By continuous video-recording, we quantified the severity of different stages of spontaneous convulsive seizures (Racine stages 3-5). Reduced epilepsy frequency, and slightly improvement of the phenotype severity were observed in a pilot number of Arx polyAla animals. Importantly, we found that Vorinostat treatment offset molecular processes linked to ARX-related targets damaged in the Arx polyAla cortex. Although further studies are indispensable to define the global impact of Vorinostat activity, these results pave the way for the design of novel therapeutic interventions for ARX pharmaco-resistant epilepsy and other early-onset genetic epilepsies
A novel promising therapeutic paradigm for the treatment of drug-resistant seizures in a genetic mouse model of developmental and epileptic encephalopathy
Verrillo L;Barra A;Miano MG
2022
Abstract
Developmental and epileptic encephalopathies (DEE) are severe forms of early onset epilepsies, usually with genetic/metabolic aetiology, characterized by drug-resistant seizures (i.e. epileptic spasms), global developmental delay or intellectual disability and characteristic EEG pattern (i.e. hypsarrhythmia). One of the monogenic causes of DEE are expansion mutations in a GCN codon repeat of the Aristaless related homeobox (ARX) gene, which leads to a polyalanine (polyA) tract elongation. Although significant progress has been made in understanding the DEE1 pathogenesis, no efficacious drugs have been identified to stop recurrent seizures. Here we report on the epilepsy behaviour analysis of the clinical mouse model of DEE, Arx polyalanine (Arx polyAla) that express the c.330ins(GCG)7 mutation through the insertion of seven GCG alanine codons in the first polyA stretch. These mice exhibit severe spontaneous tonic-clonic seizures and present a high risk for Sudden Unexpected Death in Epilepsy (SUDEP). We present promising data on in vivo post-natal treatments with the Food-Drug Administration (FDA)-approved HDAC inhibitor Vorinostat, which anticonvulsant property has been widely reported. The treatment was done by daily intraperitoneal injection for 7 days, after quantification of baseline seizure frequency. By continuous video-recording, we quantified the severity of different stages of spontaneous convulsive seizures (Racine stages 3-5). Reduced epilepsy frequency, and slightly improvement of the phenotype severity were observed in a pilot number of Arx polyAla animals. Importantly, we found that Vorinostat treatment offset molecular processes linked to ARX-related targets damaged in the Arx polyAla cortex. Although further studies are indispensable to define the global impact of Vorinostat activity, these results pave the way for the design of novel therapeutic interventions for ARX pharmaco-resistant epilepsy and other early-onset genetic epilepsiesI documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
