Clinical Trial Details
— Status: Enrolling by invitation
Administrative data
| NCT number |
NCT04309812 |
| Other study ID # |
IRB# 47711 |
| Secondary ID |
|
| Status |
Enrolling by invitation |
| Phase |
Early Phase 1
|
| First received |
|
| Last updated |
|
| Start date |
May 26, 2021 |
| Est. completion date |
July 26, 2023 |
Study information
| Verified date |
November 2022 |
| Source |
Stanford University |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
This is a placebo-controlled study of the effectiveness of transcranial direct current
stimulation (tDCS) at home to reduce seizures and EEG spikes.
Description:
Electrical stimulation is a promising new therapy to reduce seizures, but current methods
require inserting wires under the skull or into brain. This project will use direct-current
electrical stimulation pulses delivered from scalp electrodes to provide stimulation. The
goal is to reduce seizures without the need for surgery.
2. PROCEDURES:
2.1. Baseline: Upon signing of consent, subjects will have an initial screening clinic visit
with a neurological history and examination. You will record a seizure diary for one month
prior to start of stimulation.
2.2. Baseline EEGs: A 2-hour recording will be done with the 256 channel hydrogel electrocap
(currently used for clinical studies). Subjects will be maintained awake for consistency,
since sleep affects EEG activity.
2.3. Seizure Diary: The subject (and/or family) will maintain a seizure diary during the
baseline, treatment, and for one month after their final stimulation treatment. The seizure
diary will be reviewed by the study coordinator in a phone contact once per week.
2.4. Baseline antiepileptic drug levels for patients taking phenytoin, phenobarbital,
carbamazepine, valproic acid, lamotrigine or levetiracetam.
2.5. Baseline neuropsychological testing: Subjects will take baseline neuropsychological
tests, consisting of Beck Depression Index, the National Hospital Seizure Severity Scale, the
Personal Impact of Epilepsy (PIES) scale and the Montreal Cognitive Assessment basic scale.
3. Transcranial Direct Current Stimulation Treatment Procedures
3.1. tDCS: The direct current stimulus will be delivered via a commercially-available
ActivaDose transcranial direct current stimulator (or if it becomes unavailable, a
commercially available Soterix Medical device) through a saline-moistened pad placed over the
region of the seizure focus. Cathodal (negative) DC current will be delivered to the seizure
focus and anodal (positive) current over the oppositel forehead.
3.2. Ensuring comfort: Direct current stimulation will be at an intensity of 2 mA for 30
minutes per session, with slow ramp-up and ramp down of the current. This level of
stimulation is usually comfortable to most subjects. If the sensation is significantly
uncomfortable, the stimulation will be reduced to 1 mA, and if that is uncomfortable, you
will be discontinued from the study.
3.3. Except for initial, mid-study and final EEG recording and the device use training
session, this study will take place in your home. During a training session for home use you
will be made familiar with the ActivaDose operation by study staff. Features to be learned
will include:
a. Turning on the device b. Setting the stimulation to 2 mA c. Setting the stimulation
duration to 1 minute or 30 minutes. Attachment of the 2 pads (cathode and anode). e. Proper
placement of pads, careful explanation of cathode to go over the seizure zone.
f. Pad removal, disposal and device storage g. Schedule for treatments
3.4. Placebo: It is not yet clear whether short stimulation of 1 minute (SHORT) is less
effective than is longer stimulation of 30 minutes (LONG). A balanced deck of randomized
cards setting the initial treatment arm as SHORT in 15 cases and LONG in 15 cases. However,
you will receive both treatments in different months, and afterwards will have the option of
continuing with the one that works best for you (assuming that one of the treatments helps).
3.5. Schedule: After signing consent, the study will begin with one month of baseline while
keeping a daily seizure diary. During this baseline month, you will have baseline EEG
recorded and training on device use. There will then be one month of treatment SHORT or LONG,
one month no treatment "wash-out," then one-month of treatment LONG or SHORT, including the
treatment not given in the first round. Diary will be kept for one month after the second
treatment. You will be given a printed schedule of dates and the device settings to use for
each date.
3.6. Medications: During the baseline, treatment months, washout month and one month of
follow-up after treatment, efforts will be made to keep your seizure medicines constant.
However, medicines can be changed if the treating physician believes it is necessary for your
welfare
3.7 Visits: Phone visits will be made and logged one week (± 3 days) after initiating
treatment SHORT or treatment LONG. Three in-person visits will be performed: at baseline and
after completion of the two treatment months.
3.8. Follow-up testing: A 1-hour EEG will be performed during the wash-out month and after
completion of both treatment arms. The final EEG will record 2 hours of spontaneous activity,
followed by 30 minutes of Active tDCS at 2 mA, and then 30 min of subsequent recording. This
will be done to evaluate any acute EEG changes produced by tDCS. Together with the baseline
study, this will total 3 EEGs. Neuropsychological tests will be administered twice: at
baseline and after completion of all treatments.
3.9. Escape Criteria: For individual subjects, the study will be terminated for any of the
following reasons:
1. Unacceptable discomfort or pain in response to the tDCS treatment.
2. A tonic-clonic seizure occurring during a stimulation session.
3. Emergence of a first-in-life tonic-clonic seizure at any time during the study.
4. Generalized status epilepticus.
5. Tripling or more of the baseline seizure frequency.
