Synchronized Transcranial Magnetic Stimulation for PTSD

Posttraumatic stress disorder (PTSD) is a highly prevalent psychiatric disorder associated
with high degrees of comorbidity (e.g., major depressive disorder), poor quality of life, and
significant social and occupational dysfunction. Currently available evidence-based
pharmacological and psychological treatments for PTSD have only modest efficacy, and thus
further research is necessary to develop treatment approaches in order to ameliorate the
current disparity between disorder impact and prevalence, and effective therapies.

The use of non-invasive neuromodulation techniques, such as repetitive transcranial magnetic
stimulation (rTMS), in an outpatient setting, has shown to be effective in reducing symptoms
in various mental disorders, including PTSD and major depressive disorder (MDD). Research
examining the use of rTMS for PTSD still remain limited, the majority of findings pertain to
rTMS in MDD cohorts, which excluded individuals with PTSD. Given the high rate of PTSD with
MDD comorbidity, additional studies examining this comorbid population are necessary.

Furthermore, rTMS treatment parameters and duration are rather time consuming for patients,
requiring that patient travel to an outpatient facility daily, for 6 to 8 weeks, for 30 to 40
minutes each day. This can be an inconvenience and poses an additional burden for individuals
that already struggle with societal integration and social/occupational dysfunction. Thus,
further exploration and development of non-invasive brain stimulatory devices with the same
(or better) effectiveness as rTMS, that can be adapted to be utilized in an at home setting,
would revolutionize the treatment of PTSD.

The synchronized transcranial magnetic stimulation (sTMS, NeoSync Inc.) device provides the
possibility of the fore mentioned therapeutic development. The sTMS device employs 3
transversely rotating, to deliver low energy, sinusoidal magnetic fields synchronized to an
individuals' intrinsic alpha frequency (IAF). Preliminary data has shown that sTMS can
effectively reduce depressive symptoms in MDD. Additionally, the investigators' preliminary
examination of IAF in participants with comorbid PTSD and depressive symptoms, has
illuminated the feasibility of this modality as a treatment approach for PTSD comorbid with
MDD.

This study is a prospective, sham-controlled, trial of sTMS delivered to patients who are
symptomatic despite ongoing pharmacotherapy for PTSD and mood symptoms. Eligible subjects
will be randomized using to receive 4 weeks (5 daily sessions per week) of either sham or
active sTMS treatment. Clinical and self-report assessments will be completed at baseline,
sham/control series endpoint, and 1 month after the final treatment session. An optional
open-label continuation phase will be offered to all study participants who complete the
sham-control phase of this study, and additional endpoint assessments will be administered.

Inclusion Criteria:

- Must be a Veteran;

- MRI safe;

- Meet Diagnostic and Statistical Manual, Fifth Edition (DSM 5) criterion for PTSD
(acute or chronic, confirmed by the Clinician Administered PTSD Scale (CAPS) and at
least moderate severity defined by a PCL-5 score > 33); AND at least moderate
depressive symptom severity (defined by QIDS-SR score > or equal to 11) at baseline
visit. Individuals with bipolar II or otherwise unspecified who are currently in a
depressed episode are eligible;

- Baseline score of "moderately ill" or worse on the Clinical Global
Impressions-Severity (CGI-S);

- Stable psychotropic regimen for at least 6 weeks prior to baseline and willing to
maintain current dose and regimen throughout study, or no psychotropic medication at
all;

- If female and of child bearing potential, must agree to use an acceptable method of
birth control for the duration of the study treatment period;

- Be willing and able to comply with all study related procedures and visits;

- Be capable of independently reading and understanding all patient information
materials and giving written informed consent.

Exclusion Criteria:

- Pregnant or lactating, or planning on becoming pregnant within the next 3 months;

- Lifetime history of loss of consciousness (>10 minutes) due to head injury, or
lifetime history of head injury with documented evidence of brain injury;

- Current (or past) significant neurological disorders (seizure disorder, primary or
secondary central nervous system (CNS) tumors, stroke, cerebral aneurysm);

- Unstable medical illness, or significant absence of appropriate medical care;

- Current axis I primary psychotic disorder or Bipolar I disorder;

- Active (within the last month) moderate or severe substance (excluding
nicotine/caffeine) abuse disorders. Individuals on stable (>3 months), monitored
opiate agonist therapy may be included at investigator's discretion;

- Past failed treatment with rTMS or electroconvulsive therapy (ECT); any past treatment
with deep brain stimulation or vagus nerve stimulation;

- Have an active suicidal intent or plan, or in the opinion of the investigator, is
likely to attempt suicide in the next 6 months;

- Presence of condition or circumstance with potential to prevent study completion;

- Inability to obtain sufficient EEG to calibrate study device.