Major Depression Clinical Trial
Official title:
Essential Fatty Acids in Management of MDD - A Pilot Study
This is a research study to determine whether omega-3 fatty acid supplementation, when taken
with the antidepressant medication escitalopram (Lexapro), helps to improve depressive
symptoms in individuals who have major depressive disorder (MDD).
Omega-3 fatty acids are found in foods including walnuts, some fruits and vegetables, and
coldwater fish such as herring, mackerel, sturgeon, and anchovies.
Primary aims
Aim 1: To determine whether measures of essential fatty acid (EFA) membrane composition
predict symptom improvement during selective serotonin reuptake inhibitor (SSRI) treatment
of major depressive disorder.
Aim 2: To determine whether augmentation with the EFA eicosapentaenoic acid (EPA) is likely
to benefit patients who have had an inadequate improvement following four weeks of SSRI
monotherapy.
Aim 3: To determine the degree to which improvement following omega-3 supplementation in
SSRI partial responders reflects changes in the erythrocyte concentrations of EPA and DHA
and in the ratio of EPA to arachidonic acid (AA) erythrocyte concentrations.
Secondary Aim:
To determine whether relationships between changes in tissue EFA concentrations and changes
in depressive symptoms following omega-3 supplementation are mediated by changes in cytokine
activity.
Primary Hypotheses:
Hypothesis 1: After four weeks of treatment with the SSRI escitalopram Montgomery-Asberg
Depression Rating Scale (MADRS) scores will correlate positively with baseline RBC
concentrations of EPA and DHA and negatively with baseline erythrocyte ratios of AA to EPA.
Hypothesis 2: Among patients who continue to meet criteria for MDD after four weeks of
treatment, both those randomized to .7 grams and those randomized to 1.5 grams daily of EPA
supplementation will show a greater mean improvement in MADRS scores after an additional six
weeks than will those assigned to placebo supplementation.
Hypothesis 3: After patients who have had inadequate antidepressant responses to SSRI
treatment complete six weeks of augmentation with placebo, or with .7 grams or 1.5 grams per
day of EPA, a relationships will exist between final MADRS scores and both the final RBC
concentrations of DHA and EPA and the final RBC ratio of AA to EPA. These relationships will
resemble those between baseline RBC concentrations and subsequent responses to escitalopram
and will suggest therapeutic ranges for these concentrations.
Secondary Hypothesis:
Among patients with erythrocyte EPA concentrations less than 0.82% at the beginning of the
augmentation trial, the association between subsequent changes in depressive symptoms and
EPA tissue concentrations will be markedly reduced by the introduction of changes in IL-1
beta, IL-10 and PGE2 into the model.
Study Design:
Phase one is a four-week open trial and is designed to test specific response predictors. A
subset of subjects who complete phase one will enter phase two, a six-week, double-blind,
placebo-controlled trial designed to show whether eicosapentaenoic acid (EPA) is an
effective augmentation agent in patients who have had an inadequate antidepressant response.
A pilot of thirty (30) subjects, aged 18-55 years, with current major depressive disorder
who have taken not regularly taken antidepressants in the previous month. Cognitively
impaired subjects will not be included.
This is a pilot study designed to demonstrate the feasibility for an NIMH application. It is
not currently powered to statistically test the listed hypotheses.
Study outcomes/endpoints:
The primary outcomes for both phases will be the final MADRS score.
Study Procedures:
Subjects will be recruited through advertisement and through the University of Iowa
Hospitals and Clinics (UIHC) adult clinic. Advertisements will also be placed in the
newspapers of cities within a 100-mile radius of UIHC.
Screening procedures:
The study's research associate will screen calls, contact respondents, and administer the
screening to determine eligibility. Those who appear to satisfy entry criteria will be given
appointments to meet with the PI and Co-PI. If the in-person evaluation confirms the
subject's eligibility, he or she will be given a consent form and be invited to ask any
remaining questions he or she might have. The protocol could begin at that visit.
Study Intervention:
Active study agents: Escitalopram and eicosupentaenoic acid (EPA). A variety of
antidepressants are available for the treatment of Major Depressive Disorder (MDD). A number
of psychotherapeutic approaches also have demonstrated effectiveness. Potential subjects
could receive both escitalopram and EPA without participating in the study.
Placebo study agents: Placebo capsules will match the EPA capsules.
Storage:
Drug will be locked and maintained in the medical education building. Data forms and
computerized data will be stored in the University of Iowa Medical Education Building.
Offices and cabinets will be locked, computer files will be password protected. The lab of
Arthur Spector, M.D. will analyze the blood samples.
Administration:
In phase one, subject will be given a 4 week supply of 10 mg escitalopram (Lexapro) and
instructed to take one pill a day for 4 weeks.
If eligible for phase 2 of the study, subject will continue to take 10 mg of escitalopram
but will also be randomly assigned to take, in addition, either 0.7 grams or 1.5grams of the
EPA or a placebo.
** If depression symptoms have improved by greater than 50% at the end of week 4, subject
will be given a 1 month supply of escitalopram and will be assisted in obtaining psychiatric
care in their area.
If depression symptoms have not improved by greater than 50% at the end of week 4 subject
will be invited to participate in Phase 2 of the study.
The protocol will begin with the administration of a structured diagnostic interview, the
Structured Clinical Interview for DSM IV Diagnosis (SCID), and two depression rating scales,
the Montgomery Asburg Depression Rating Scale (MADRS) and the Hamilton Rating Scale (HRS).
Two tubes of blood will be drawn, one for erythrocyte EFA concentration determination and
the other for quantification of inflammatory markers (c-reactive protein). Subjects will
then be supplied with a one-month supply of escitalopram (Lexapro) with instructions to take
one 10mg capsule each morning. Return visits at two weeks and four weeks will be scheduled
and subjects will be instructed to return with any remaining medication.
Subjects will be contacted at weekly intervals. During a brief telephone conversation he or
she will ask whether the subject has any questions or has experienced any troublesome side
effects.
Those who meet the criteria for inadequate escitalopram response described above will be
invited to participate in a six-week trial of supplemental omega-3. Subjects will continue
taking escitalopram at the previous dose of 10mg daily but will be randomly assigned to
take, in addition, either 0.7 grams or 1.5 grams of the eicosapentaenoic acid (EPA) or a
placebo.
Visits for phase 2 will be scheduled at weeks 6, 8, and 10. At week 4 and 10 blood samples
for erythrocyte EFA concentrations and cytokine determinations will be drawn. MADRS will be
rated on these visits.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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