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Add-on
Gabapentin for Refractory Seizures in Patients with Brain
Tumours
James R Perry and Carol Sawka
Abstract:
Background: Seizures associated with
intracranial neoplasms are occasionally refractory to conventional
anti-epileptic drugs. Gabapentin (GBP) is one of several
novel anti-epileptic drugs effective as an add-on therapy
for intractable seizures but has not been studied in patients
with cerebral tumours. Patients and Methods:
We used GBP in a open-label add-on fashion to treat 14 patients
with intractable seizures associated with intracranial tumours
including four glioblastomas, four metastases, three recurrent
glioblastomas, and one each of anaplastic and low grade
astrocytoma and meningioma. GBP was added if optimization
of pre-existing therapy failed and was titrated until seizures
were controlled. Results: One patient experienced
adverse drowsiness. Follow-up ranged from 3-24 weeks during
which time 7 patients died from disease progression. Concurrent
therapy included dexamethasone in eight, cranial irradiation
in four, and radiosurgery in one. Responder rate (number
with at least 50% fewer seizures) was 100% and persisted
throughout follow-up. Complete resolution of seizures occurred
in 8/14 patients. Conclusions: GBP was well
tolerated in patients with brain tumours. Seizure frequency
was reduced in all patients and efficacy persisted over
time; however, the mechanism of this improvement is unclear.
Concurrent therapy, regression of frequency to the mean,
and the lack of controls may account for apparent benefit.
In addition, because GBP may interact with a leucine-related
neuronal binding site we also speculate that this novel
mechanism of action may have been enhanced in our patients
due to the abnormal blood-brain barrier associated with
cerebral tumours. Further investigation and a controlled
trial are warranted.
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Can.
J. Neurol. Sci. 1996; 23: 128-131
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