Major Depressive Disorder Clinical Trial
Open label placebo treatment has been tried for irritable bowel syndrome (Kaptchuk et al,
2010), where three weeks of open label placebo proved superior to a wait-listed control
group. Another pilot study demonstrated efficacy in treating children suffering from ADHD
with open label placebo treatment (Sandler & Bodfish, 2007). Recent work has shown that
placebo openly given can have significant analgesic effects for acute migraines (Kam-Hansen
et al, 2014) and for experimentally-induced pain (Schafer at al, 2015). A preliminary
attempt to treat depression with open label placebo proved the feasibility of such a study,
but was too small and brief for conclusive results (Kelley et al, 2012).
We provide here the protocol for a study to assess the effect of open label placebo
treatment for depression.
participants will be recruited through advertisements in the traditional and on-line press,
and via mental health care workers in local clinics. The psychiatrists in the study team
will also have the option to access to the waiting list of outpatient clinics at the
Shalvata Mental Health Center, and recruit patients (who's intake appointment in the
outpatient clinic is expected to take place in more than 2 months) to the study via phone or
face to face in the clinic. If a subject is already taking antidepressant treatment he can
be recruited immediately to the study. If a subject is not taking an antidepressant
treatment, and in his examination he is diagnosed with depression, the investigator will
advice him to approach an outpatient clinic and start taking antidepressant medication. If
the subjects refuses to use medications he will be recruited to the study medication-free.
Patients will be invited to participate in the study and the following wording will be used:
"we invite you to participate in a novel mind-body study harnessing placebo effects for the
treatment of depression. In the study you will recieve, either immediately or following a
waiting period, placebo (inert) tablets. There will be no active component in the tablet,
but there is a good chance that it will alleviate some of the depressive symptoms.
Furthermore, recent scientific evidence suggests that placebo tablets can initiate healthy
responses even if a person knows they are placebos".
Each participant will provide signed informed consent. Each subject will receive a letter to
his personal physician or psychiatrist in the community/hospital. Additionally, the study
team will also contact the personal physician and inform him of the study. Subjects will
continue their psychiatric follow-up and treatment as usual during the whole period of the
study. If the study team recognized a suicidal deterioration the personal
physician/psychiatrist will be notified immediately via phone. If a subject is currently
without psychiatric follow-up, he will examined during the assessment points (every 2 weeks)
of the study protocol by one of the physicians of the study team.
Before the first session, each participant will be randomized to one of two possible
interventions: either 8 weeks of open label placebo, or 4 weeks of waitlist followed by four
weeks of open label placebo.
The randomization procedure will be stratified to account for two groups of subjects: those
currently on a stable dose of medication, and those currently receiving no medication.
Therefore, each time a subject from one of these groups is randomized to one of the two
interventions (open label placebo or wait list), the next subject from the same group will
be assigned to the other intervention. By this method, we will obtain the same proportion of
medicated and unmedicated patients in each of the two intervention arms.
At the first session, the participant positive expectation and commitment will be promoted
by discussing with the participant the following four points: (a) in research, placebos have
been found to be safe in terms of side-effects and roughly 80% as effective as
antidepressants; (b) recent research suggests that a patient can benefit from a placebo even
when he knows that he is taking a placebo; (c) placebos appear to promote automatic
self-healing processes, possibly through classical conditioning ; just taking tablets can
cause the release of neurotransmitters and activate specific regions of the brain related to
depression] (d) placebo-treated patients who adhere to the tablet regimen have better
outcomes, and therefore the placebos should be taken faithfully, and (e) positive
expectations enhance placebo effects, but it is perfectly normal to have doubts or disbelief
and won't interfere with the effect.
At the end of the first session, the researcher will open an envelope which will reveal to
researcher and participant to which group the latter has been randomized. Both treatment arm
and no-treatment control will have identical patient-provider interactions and be of equal
length. Those in the waitlist group will be encouraged to continue in the study.
The placebo will be a colored tablet. Each participant will be enjoined to take two capsules
in the morning, and two in the evening.
After four weeks, the placebo group will continue with a second four week period of placebo
treatment, and the waitlist group will start to receive 4 weeks of placebo treatment.
;
Allocation: Non-Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Crossover Assignment, Masking: Open Label, Primary Purpose: Treatment
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