Epilepsy Clinical Trial
Official title:
Neuroimaging Predictors of Treatment Failure in Adult New-onset Epilepsy
Epilepsy, defined as recurrent, unprovoked seizures, is a common condition, affecting 0.5-1%
of the general population. People with uncontrolled epilepsy suffer poor health and
increased mortality due to their condition. They frequently experience social stigma and are
socioeconomically disadvantaged. It is therefore imperative to help them gain control of
their seizures as quickly as possible. A wide range of antiepileptic drugs (AEDs) has become
available to treat people with epilepsy. However, despite maximal therapy, approximately
20-40% show pharmacoresistance (PR) and thus continue to have seizures.
We do not understand why a significant proportion of people with epilepsy have PR. For any
given patient presenting with a first unprovoked seizure, we are unable to predict PR at the
time of presentation. At least 2 different AEDs must be tried at maximum doses for a year
before we can diagnose PR. At this point, surgical therapies become an increasingly urgent
consideration.
Retrospective magnetic resonance imaging (MRI) studies in the chronic stages of epilepsy
have shown that patients with PR are more likely to have focal structural lesions in the
brain, and in particular to have signs of damage to the hippocampi. For example, there are
retrospective data suggesting that a decreased hippocampal N-acetylaspartate (NAA)/creatine
ratio (measured by magnetic resonance spectroscopy [MRS]) and hippocampal atrophy
(determined by hippocampal volumetry) correlate with PR. However, it is not clear whether
these findings reflect the underlying pathophysiology of PR, or simply reflect the effects
of chronic seizures and chronic drug treatment on the brain.
The First Seizure Clinic at the Halifax Infirmary represents a unique opportunity for
prospective, longitudinal studies of patients who present with a first seizure or with newly
diagnosed epilepsy. In these patients, advanced neuroimaging techniques at presentation
might show changes that truly reflect the underlying pathophysiology of PR, rather than
changes that develop as a consequence of prolonged seizures and drug treatment. Neuroimaging
follow-up might help us to understand the pathophysiologic changes that accompany the
evolution of PR. Ultimately, it is our hope to combine neuroimaging features and clinical
features of patients with PR in a predictive model that would help us to predict PR at
presentation.
n/a
Observational Model: Cohort, Time Perspective: Prospective
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