Major Depression Clinical Trial
Official title:
Vortioxetine for the Treatment of Major Depression and Neuropsychiatric Co-morbidities After Traumatic Brain Injury (TBI)
Traumatic brain injury (TBI) is a major public health problem with an annual incidence of
about 1.7 million per year. TBI is associated with various long-term morbidities. Among
them, psychiatric disturbances are the major cause of chronic disability and poor quality of
life. Major depression is the common psychiatric sequela post TBI with rates ranging from
13% at 1 year to 60% at 8 years after TBI. Major depression after TBI (henceforth referred
to as TBI depression) is often associated with comorbid neuropsychiatric symptoms (NPS) such
as anxiety, aggression, substance abuse and cognitive deficits that often makes treatment
difficult. Despite increased rates of depression, there is no Food and Drug Administration
(FDA) approved drug/s for its treatment.
The investigators propose to address these limitations by use of a novel serotonergic agent,
vortioxetine, which has a multimodal mechanism of action through serotonin transporter
(SERT) inhibition, 5-hydroxytryptamine (5-HT)3, 7, and 1D receptor antagonism, 1B receptor
partial agonism, and 1A receptor agonism.
Overarching Goal: The overarching goal of the proposed pilot study is to determine the
effectiveness and safety of vortioxetine for the treatment of post-TBI depression and
co-morbid NPS.
Study Design: The study design will include a DBPCT of 30 TBI patients of all severities who
meet the DSM 5 criteria for major depression. A total of 150 will be consented to allow for
screen failures. Written informed consent will be obtained from these patients. Subjects
will be followed for a total of 12 weeks. Subjects will be randomized to either the
vortioxetine arm (N=15) or placebo arm (N=15). The treatment group will receive vortioxetine
10mg per day, which will be increased to 20 mg or decreased to 5 mg, if deemed clinically
necessary, at week 4 or 8. Subjects will have a total of 4-5 visits: Baseline evaluation (1
or 2 visits) and follow-up visits at weeks 4, 8 and 12. Well-validated psychiatric
instruments will be used to compare the effectiveness of vortioxetine versus placebo
treatment at week 12 compared to baseline Relevance: This study has the potential to provide
strong preliminary evidence for the use of vortioxetine as a safe and novel agent for
treatment of TBI depression and its psychiatric co-morbidities. If found to be effective,
results from this study can be used to design larger studies and also determine brain
changes associated with its use via neuroimaging.
In this study the investigators propose to recruit 30 outpatients with TBI of varying
degrees of severity who also meet DSM 5 criteria for major depression. The investigators
will screen as many potential subjects as possible to get a total of 30 participants who
meet the study criteria and complete the study ( Total 30 study completers). Written
informed consent will be obtained from all participants prior to collection of any data.
Participants will be evaluated using well validated psychiatric instruments Participants
will be recruited from several sources: (1) Brain Injury Clinic at Johns Hopkins Bayview
Medical Center; (2) referral from other Hopkins outpatient clinics; (3) Brain injury support
groups organized by the Brain Injury Association of Maryland, and (4) Advertisements placed
in local newspapers and (5) Trial Facts - an online recruiting source. The study sites will
be at the Geriatric & Neuropsychiatry clinics at Johns Hopkins Bayview Medical Center.
Overarching Goal: The overarching goal of the proposed pilot study is to determine the
effectiveness and safety of vortioxetine for the treatment of post-TBI depression and
co-morbid neuropsychiatric symptoms (NPS).
Study Design: The study design will include a Double Blinded Placebo Controlled Trial
(DBPCT) of 30 TBI patients of all severities who meet the DSM 5 criteria for major
depression. A total of 150 will be consented to allow for screen failures. Written informed
consent will be obtained from these patients. Subjects will be followed for a total of 12
weeks. Subjects will be randomized to either the vortioxetine arm (N=15) or placebo arm
(N=15). The treatment group will receive vortioxetine 10mg per day, which will be increased
to 20 mg or decreased to 5 mg, if deemed clinically necessary, at week 4 or 8. Subjects will
have a total of 4-5 visits: Baseline evaluation (1 or 2 visits) and follow-up visits at
weeks 4, 8 and 12.
Well-validated psychiatric instruments will be used to compare the effectiveness of
vortioxetine versus placebo treatment at week 12 compared to baseline for the treatment of
major depression and its neuropsychiatric co-morbidities.
Relevance: This study has the potential to provide strong preliminary evidence for the use
of vortioxetine as a safe and novel agent for treatment of TBI depression and its
psychiatric co-morbidities. If found to be effective, results from this study can be used to
design larger studies and also determine brain changes associated with its use via
neuroimaging. Depression is common in other neurological disorders such as stroke, multiple
sclerosis, Parkinson's disease, and dementia syndromes. Results from this study can shed
light in the management of depression in other neurological disorders.
;
Allocation: Randomized, Endpoint Classification: Pharmacokinetics/Dynamics Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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