Methylphenidate for the Treatment of Epilepsy-related Cognitive Deficits
NCT ID: NCT04419272
Last Updated: 2025-04-02
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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RECRUITING
PHASE4
226 participants
INTERVENTIONAL
2023-08-14
2027-09-30
Brief Summary
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Detailed Description
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The primary aim is to evaluate the efficacy of MPH for the treatment of attentional dysfunction in subjects with epilepsy. It is expected that subjects will have improved attention when taking MPH compared to placebo, measured by the Conner's Continuous Performance Test (CPT). The effects of MPH on other cognitive functions that rely in part on attention, including a composite measure of memory (MCG Paragraph Test), psychomotor speed (Symbol Digit Modalities Test), and divided attention, psychomotor speed, and response inhibition (Stroop Color Word Interference Test), will be ascertained. Improved performance when taking MPH compared to placebo is expected. Finally, the study will establish the effect of MPH on overall quality of life. It is hypothesized that there will be improvement in self-reported quality of life with MPH, but no change with placebo, as assessed by the Quality of Life in Epilepsy Patient Inventory.
We will evaluate the safety of MPH compared to placebo with respect to seizure frequency. Secondary analyses will determine continued efficacy over an open-label period. To control for practice effects, cognitive performance will be compared to healthy subjects and epilepsy patients without cognitive complaints, who will complete the repeated cognitive measures but remain untreated for the duration of the trial.
Conditions
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
QUADRUPLE
Study Groups
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Methylphenidate
Subjects who will receive methylphenidate in the double-blinded period; when assigned to the active drug, the dosage of MPH will begin at 10mg twice per day, at 8am and 12pm, for one week. The dosage will then increase to 20mg twice daily, at 8am and 12pm, for the next 7 weeks.
Methylphenidate
10mg twice per day, at 8am and 12pm, for one week, then increased to 20mg twice daily, at 8am and 12pm, for the next 7 weeks during the double-blinded period.
Placebo
Subjects who will receive placebo in the double-blinded period; when assigned to receive the placebo during the double-blinded period, subjects will be given a sugar pill for 8 weeks. The sugar pill will be taken twice per day, at 8am and 12pm.
Placebo
When assigned to receive the placebo during the double-blinded period, subjects will be given a sugar pill for 8 weeks. The sugar pill will be taken twice per day, at 8am and 12pm.
Open-Label Methylphenidate
All subjects will be offered open-label methylphenidate during Weeks 9-16. the dosage of MPH will begin at 10mg twice per day, at 8am and 12pm, for one week. The dosage will then increase to 20mg twice daily, at 8am and 12pm, for the next 7 weeks.
Methylphenidate
During the open-label extension phase, dosing will begin at 10mg twice per day, at 8am and 12pm, for one week. The dosage will then increase to 20mg twice daily, at 8am and 12pm, for the next 7 weeks.
Interventions
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Methylphenidate
10mg twice per day, at 8am and 12pm, for one week, then increased to 20mg twice daily, at 8am and 12pm, for the next 7 weeks during the double-blinded period.
Placebo
When assigned to receive the placebo during the double-blinded period, subjects will be given a sugar pill for 8 weeks. The sugar pill will be taken twice per day, at 8am and 12pm.
Methylphenidate
During the open-label extension phase, dosing will begin at 10mg twice per day, at 8am and 12pm, for one week. The dosage will then increase to 20mg twice daily, at 8am and 12pm, for the next 7 weeks.
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
Participants will include adult subjects with focal-onset epilepsy, based on clinical history, imaging studies and ictal and/or interictal EEG interpreted by a clinical epileptologist. Seizures may be symptomatic, idiopathic, traumatic, or non- traumatic in etiology. Subjects must have self-reported cognitive dysfunction. Subjects must also meet the following eligibility criteria:
* Age 18 years of age or older;
* Capacity to provide informed consent;
* Ability to live independently and complete activities of daily living;
* Stable seizure frequency at the time of enrollment, such that the subject's treating physician does not believe a change in ASM regimen to be warranted during the trial (ASMs should remain unchanged during the 16 weeks of participation unless absolutely required clinically due an unanticipated change in seizure frequency or severity);
* Fluency in written and spoken English.
2. CONTROLS \*DO NOT UNDERGO ANY DRUG OR PLACEBO INTERVENTION Two additional subject groups will be included, to control for effects of repeated testing in the open-label extension phase: healthy subjects and epilepsy patients without cognitive complaints, who will not receive the study drug at any point during the study. Epilepsy patients without cognitive deficits must otherwise meet all of the above criteria.
* Age 18 years or older;
* Capacity to provide informed consent;
* Ability to live independently and complete activities of daily living;
* Fluency in written and spoken English.
Exclusion Criteria
Subjects with epilepsy with or without cognitive complaints will be excluded from participation for:
* Psychogenic, non-epileptic spells
* Delirium in the past year
* Other progressive neurologic illness (i.e., malignant brain tumor). A benign, stable neoplasm with no plans for resection will not be cause for exclusion.
* A history of alcohol or illicit drug abuse;
* Generalized tonic-clonic or other generalized motor seizure(s) within 48 hours or focal-onset seizures with impaired awareness within 24 hours of neuropsychological testing;
* Status epilepticus in the past year;
* Neurosurgery within the past 6 months;
* Suicide attempt in the past year and/or high-risk suicide flag in the medical record;
* Psychotic disorders
* Severe anxiety (\>26 on the Beck Anxiety Inventory \[BAI\]) and impulse control disorders;
* Untreated sleep disorders;
* Use of narcotic or other sedating medications within 6 hours of testing (i.e., diphenhydramine);
* Concurrent severe major medical illness (i.e., cancer requiring chemotherapy or resection)
* Prior transient ischemic attack (TIA) or stroke
Subjects with epilepsy will also be excluded for a diagnosis of dementia (i.e., Alzheimer's disease). Subjects with epilepsy and cognitive complaints must have a MoCA score of 18 or greater. Subjects with epilepsy and no cognitive complaints must have a MoCA score of 26 or greater.
* Current pregnancy or pregnancy planned during the trial
* Breastfeeding
* Concurrent treatment with a monoamine oxidase inhibitor (MAOI) or MAOI use within 14 days of beginning the trial;
* Structural cardiac abnormalities, cardiomyopathy, serious arrhythmias, or coronary artery disease (including a history of myocardial infarction, cardiac stent placement, coronary artery bypass graft surgery, or angina);
* Bipolar disorders;
* Concurrent use of medications for erectile dysfunction (e.g., tadalafil, sildenafil);
* Use of medications that may lower seizure threshold (e.g., tramadol, bupropion) or induce psychosis (i.e., varenicline);
* Known allergy or intolerance to MPH;
* Uncontrolled hypertension;
HEALTHY CONTROLS
Healthy controls will be excluded based on the following criteria:
* History of seizures, epilepsy, or psychogenic, non-epileptic spells;
* Diagnosis of dementia (i.e., Alzheimer's disease), MoCA score of \<26;
* Delirium in the past year;
* Other progressive neurologic illness (i.e., malignant brain tumor);
* Prior moderate or severe traumatic brain injury (TBI);
* Mild TBI within the past 6 months;
* A history of alcohol or illicit drug abuse;
* Suicide attempt in the past year and/or high-risk suicide flag in the medical record;
* Psychotic, severe anxiety (BAI \>26), or impulse control disorders;
* Untreated sleep disorders;
* Use of narcotic or other sedating medications within 6 hours of testing;
* Ongoing major neurological or medical illness (i.e., cancer requiring chemotherapy or resection);
* Prior TIA or stroke;
18 Years
ALL
Yes
Sponsors
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VA New York Harbor Healthcare System
FED
Portland VA Medical Center
FED
Miami VA Healthcare System
FED
VA Boston Healthcare System
FED
VA Office of Research and Development
FED
Responsible Party
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Principal Investigators
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Beth A Leeman-Markowski, MD
Role: PRINCIPAL_INVESTIGATOR
VA NY Harbor Healthcare System, New York, NY
Locations
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Miami VA Healthcare System, Miami, FL
Miami, Florida, United States
VA Boston Healthcare System Jamaica Plain Campus, Jamaica Plain, MA
Boston, Massachusetts, United States
VA NY Harbor Healthcare System, New York, NY
New York, New York, United States
VA Portland Health Care System, Portland, OR
Portland, Oregon, United States
Countries
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Central Contacts
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Facility Contacts
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Other Identifiers
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CX002474
Identifier Type: OTHER
Identifier Source: secondary_id
NURD-003-22S
Identifier Type: -
Identifier Source: org_study_id
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