Finding a better drug for epilepsy: the mTOR pathway as an antiepileptogenic target.

[cowden syndrome]

The mammalian target of rapamycin (mTOR ) signaling pathway regulates cell growth , differentiation , proliferation , and metabolism . Loss -of-function mutations in upstream regulators of mTOR have been highly associated with dysplasias , epilepsy , and neurodevelopmental disorders . These include tuberous sclerosis , which is due to mutations in TSC 1 or TSC 2 genes ; mutations in phosphatase and tensin homolog (PTEN ) as in Cowden syndrome , polyhydramnios , megalencephaly , symptomatic epilepsy syndrome (PMSE ) due to mutations in the STE 20 -related kinase adaptor alpha (STRADalpha ); and neurofibromatosis type 1 attributed to neurofibromin 1 mutations . Inhibition of the mTOR pathway with rapamycin may prevent epilepsy and improve the underlying pathology in mouse models with disrupted mTOR signaling , due to PTEN or TSC mutations . However the timing and duration of its administration appear critical in defining the seizure and pathology-related outcomes . Rapamycin application in human cortical slices from patients with cortical dysplasias reduces the 4 -aminopyridine-induced oscillations . In the multiple -hit model of infantile spasms , pulse high -dose rapamycin administration can reduce the cortical overactivation of the mTOR pathway , suppresses spasms , and has disease-modifying effects by partially improving cognitive deficits . In post-status epilepticus models of temporal lobe epilepsy , rapamycin may ameliorate the development of epilepsy -related pathology and reduce the expression of spontaneous seizures , but its effects depend on the timing and duration of administration , and possibly the model used . The observed recurrence of seizures and epilepsy -related pathology after rapamycin discontinuation suggests the need for continuous administration to maintain the benefit . However , the use of pulse administration protocols may be useful in certain age-specific epilepsy syndromes , like infantile spasms , whereas repetitive-pulse rapamycin protocols may suffice to sustain a long -term benefit in genetic disorders of the mTOR pathway . In summary , mTOR dysregulation has been implicated in several genetic and acquired forms of epileptogenesis . The use of mTOR inhibitors can reverse some of these epileptogenic processes , although their effects depend upon the timing and dose of administration as well as the model used .