Filamin A Inhibition Reduces Seizure Activity in a Mouse Model of Focal Cortical Malformations
Abstract number :
974
Submission category :
7. Antiepileptic Drugs / 7A. Animal Studies
Year :
2020
Submission ID :
2423307
Source :
www.aesnet.org
Presentation date :
12/7/2020 1:26:24 PM
Published date :
Nov 21, 2020, 02:24 AM
Authors :
Longbo Zhang, Yale University; Tianxiang Huang - Yale University; Shannon Teaw - Yale University; Lena Nguyen - Yale University; Lawrence Hsieh - Yale University; Xuan Gong - Yale University; Lindsay Burns - Cassava Sciences Inc.; Angelique Bordey - Yale
Rationale:
Epilepsy treatments for patients with mechanistic target of rapamycin (mTOR) disorders, such as tuberous sclerosis complex (TSC) or focal cortical dysplasia type II (FCDII), are urgently needed. In these patients, the presence of focal cortical malformations is associated with the occurrence of lifelong epilepsy, leading to severe neurological comorbidities.
Method:
We show that the expression of the actin cross-linking protein filamin A (FLNA) is increased in resected cortical tissue that is responsible for seizures in patients with FCDII and in mice modeling TSC and FCDII with mutations in phosphoinositide 3-kinase (PI3K)-ras homolog enriched in brain (Rheb) pathway genes. Then we test whether targeting FLNA with either short hairpin RNAs or the small molecule PTI-125 can reduce seizures in TSC or FCDII mice model.
Results:
Normalizing FLNA expression in these mice through genetic knockdown limited cell misplacement and neuronal dysmorphogenesis, two hallmarks of focal cortical malformations. In addition, Flna knockdown reduced seizure frequency independently of mTOR signaling. Treating mice with a small molecule targeting FLNA, PTI-125, before the onset of seizures alleviated neuronal abnormalities and reduced seizure frequency compared to vehicle-treated mice. In addition, the treatment was also effective when injected after seizure onset in juvenile and adult mice.
Conclusion:
These data suggest that targeting FLNA with either short hairpin RNAs or the small molecule PTI-125 might be effective in reducing seizures in patients with TSC and FCDII bearing mutations in PI3K-Rheb pathway genes.
Funding:
:This work was supported by NIH R01 NS093704 (A.B.), R61 NS111074 (A.B.), Swebilius Foundation (A.B.), National Natural Science Foundation of China 81671123 (L.Z.), and American Epilepsy Society postdoctoral fellowship (L.H.N.).
Antiepileptic Drugs