Depression Clinical Trial
Official title:
Verstärkung Der Therapeutischen Wirkung Von Schlafentzug Durch Modafinil - Eine Doppelblinde, Randomisierte, Placebokontrollierte Monozentrische Studie Der Phase II (Enhancing the Therapeutic Efficacy of Sleep Deprivation by Modafinil - a Double Blind, Placebo-controlled Monocentric Phase II Study)
The study aims to investigate whether the administration of the stimulant modafinil during a 40 hour sleep deprivation period in depressed patients can intensify the antidepressant effect of the sleep deprivation as assessed by a reduction in the Hamilton Depression score (HAMD, 6-item version). We postulate that this also correlates with a reduction of the polysomnographically assessed overall amount of sleep during this period.
In about 60 % of depressed patients, sleep deprivation has an acute therapeutic effect. The
effect appears within very few hours; this is different from all other antidepressant
treatments. However, in most cases patients relapse after the subsequent night's sleep (Wu &
Bunney 1990).
The antidepressant mechanism of action of sleep deprivation is not known as yet; several
hypotheses are presented and discussed in various review articles (Wiegand 1995; Kasper &
Möller 1996; Wirz-Justice & van den Hoofdakker 1999; Gillin et al. 2001; Ringel & Szuba
2001; Giedke & Schwärzler 2002). At present, the following general hypotheses are most
discussed:
1. Sleep deprivation exerts its effect by activating or intensifying an antidepressant
"pro-cess". This "process" may be dopaminergic or serotonergic transmission, thyroid
function etc.
2. Sleep deprivation inactivates a hypothetic "depressiogenic" substance which is produced
during sleep.
3. Sleep deprivation reduces the central nervous cholinergic transmitter activity and
restores the balance between cholinergic and aminergic transmitter systems.
4. Sleep deprivation acts by preventing sleep during a "critical" or "vulnerable" phase of
circadian rhythms; there are various chronobiological assumptions which can specify
such a "critical phase".
Several studies tried to indentify predictors of response to sleep deprivation in order to
clarify the mechanism of action. Among clinical predictors is a symptom pattern with
"endogenous" or "melancholic" traits and the presence of pronounced diurnal variations of
mood, and a behaviour pattern pointing to an elevated level of arousal or activity. Another
predictor is a pronounced sleep disturbance during the baseline night. Among the many
neuroendocrine and neurohumoral factors which have been studied, only elevated thyroid
hormones turned out to be a predictor for response to sleep deprivation. PET and SPECT
studies have convergently demonstrated an elevated metabolism in parts of the limbic system
(e.g., the anterior cingulum) at baseline in responders. These findings do not yet allow
conclusions with respect to the neurotransmitter systems involved.
Wiegand et al. (1993) investigated whether scheduled daytime naps can induce relapses after
successful sleep deprivation therapy. The timing of the nap turned out to be a crucial
factor; nap sleep duration and sleep structure during naps were less important.
The majority of studies in this field suffers from a methodological problem: there is no
objective continuous polysomnographic measurement of sleep. The continuous absence of sleep
during the sleep deprivation period is thus not documented. It is known from sleep
deprivation studies in healthy probands that during prolonged sleep deprivation, short sleep
episodes ("microsleep") occur frequently. Hemmeter et al. (1998) were the first to
demonstrate that also in depressed patients undergoing sleep deprivation, microsleep occurs
and tends to prevent the antidepressant effect. Data from a recently finished study of our
group point into the same direction (partly published in Wiegand et al. 2002).
To further elucidate this question, an experimental procedure appears useful where the
occurrence of sleep episodes during the sleep deprivation period is suppressed as far as
possible by the vigilance enhancing drug modafinil.
The study aims to investigate whether the administration of modafinil or placebo during a 40
hour sleep deprivation period in depressed patients can intensify the antidepressant effect
of the sleep deprivation.
This study is a basic science study that aims to provide information on the therapeutic
mechanism of sleep deprivation in depression and on the reoccurence of depressive symptoms
in case of intermittent short sleep episodes.
Primary Hypothesis:
There is a significant reduction on the HAMD-6 scale between baseline and 24 h later (at the
mornings before and after one night of sleep deprivation)
Secondary Hypotheses:
1. The amount of "responders" (50% of reduction on the HAMD-6 scale) is significantly
greater in the modafinil than in the placebo group.
2. The primary hypothesis and the first secondary hypothesis are also assessed by a
self-rating scale of global mental state (Befindlichkeitsskala (Bf-s)) and by the
Stanford Sleepiness Scale.
3. The overall amount of sleep assessed by polysomnography is smaller in the modafinil
group as compared to the placebo group during the 40 h sleep deprivation period.
4. The group differences in HAMD-6 ratings are parralleled by differences in the overall
amount of sleep during the 40 h sleep deprivation period.
5. There are group differences (Modafinil versus Placebo) on a comprehensive
neuropsychological battery taken at baseline and 24 h later (at the mornings before and
after one night of sleep deprivation)
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Basic Science
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