Post Traumatic Stress Disorder Clinical Trial
Official title:
A Pilot Study to Examine Deep Brain Stimulation (DBS) in the Basolateral Nucleus (BLn) of the Amygdala for the Management of Symptoms in Veterans With Chronic and Treatment-Refractory Combat-related Post-Traumatic Stress Disorder (PTSD)
The purpose of this study is to determine whether deep brain stimulation of the basolateral nucleus (BLn) of the amygdala, on both sides of the brain, can safely reduce symptoms of post-traumatic stress disorder (PTSD) in combat veterans whose condition has not improved despite extensive treatment with currently available medication and psychotherapy interventions.
For this pilot feasibility study, combat veterans whose PTSD has been associated with severe
symptomatic suffering and functional impairment, despite treatment with all currently
available pharmacological and psychotherapeutic treatments, will be recruited from clinics
at a large, academically affiliated VA facility. An extensive screening over an extended
baseline by the study psychiatrist and neurosurgeon will be conducted using standard
interviews and clinical rating scales. Eligible subjects are required to have a cohabiting
significant other willing to participate in safety and function monitoring throughout the
study.
After successful completion of baseline eligibility requirements, comprehensive
neuropsychological testing will be performed, as will structural MRI and FDG PET/CT of the
amygdala, insula and medial Prefrontal cortex. PET/CT will be performed and analyzed by a
nuclear medicine specialist collaborator familiar with this type of imaging research. Six
consenting subjects meeting all eligibility criteria will then receive bilateral basolateral
nucleus of the amygdala (BlnA) implantation of Medtronic Activa Primary Cell (PC)
implantable deep brain stimulator systems (purchased through the VA Merit Review Grant) by
functional neurosurgeons specialized in the procedure. This will be done during a 3-4 day
inpatient stay on the VA Greater Los Angeles Neurosurgical Service. After a month of weekly
safety monitoring with stimulators off, subjects will be will be hospitalized for 1 day on
the Neurology Service's electroencephalography (EEG) telemetry unit, under the care and
supervision of an epilepsy specialist neurologist who is a co-investigator in the study, for
stimulator initiation. Stimulator settings will be adjusted by the study clinical
neurophysiologist while patients are monitored by the study neurologist and psychiatrist.
Only stimulator settings that do not cause epileptiform discharges, or potentially
significant adverse psychiatric or medical (e.g., blood pressure, heart rate) changes will
be used over the subsequent long-term follow-up.
After the EEG telemetry safety check, subjects will be randomized (3/3) to either have their
stimulators turned on then (Week 0), or 3 months later (week 12). This staggered onset
double-blind design has been used in other DBS trials in psychiatry. After week 0, for the
next 2 years, subjects will be followed at regular intervals (weekly for 5 months, then
monthly for 7 months, then quarterly for 12 months) by a psychiatrist, neurosurgeon,
neurologist and neurophysiologist who will conduct an extensive battery of psychiatric and
neurological testing (including periodic EEG recordings), as well as significant other
interviews, while stimulator settings are adjusted based on standardized rating scale
outcomes and adverse effects so as to optimize treatment outcome. The principal study
hypothesis is that the symptomatic and functional benefits of chronic stimulation will
outweigh the risks and adverse-effects, and that symptomatic improvement will be greater,
without unacceptable adverse effects, in subjects with week 0, compared to week 12
stimulator initiation. Neuropsychological testing will be repeated after 6 months of
stimulation to assess changes in cognitive function. Functional neuroimaging with PET/CT
will be repeated after a year of stimulation to assess changes in the activity of brain
regions known to function abnormally in PTSD.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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