Bipolar Disorder Clinical Trial
Official title:
Double Blind,Randomized, Placebo Controlled Trial of Adjunctive Tianeptine in the Treatment of Bipolar Depression
One of the main challenges in the treatment of Bipolar Disorder (BD) is to achieve better
functioning outcomes after syndromal recovery. Even treatment-responsive patients, who
remain symptomatically well for extended periods of time, frequently demonstrate
sub-threshold symptoms and continuing psychosocial morbidity and cognitive impairment. The
cognitive impairment that persists during interepisode periods stands out as a major
correlate of functional impairment, and may be a core aspect of the BD pathophysiology.
In this context, tianeptine stands out as a therapeutic agent with unique properties, which
match most of the conditions found in BD.
This is an enriched maintenance study of the use of tianeptine as an adjunctive therapy in
bipolar depression. All participants will receive tianeptine in an open label manner for a
period of two months, following which they will be assigned randomly to the treatment with
tianeptine or placebo in a double-blind fashion for six months. All patients will remain on
treatment as usual for the duration of the trial. Along with clinical response, the
investigators will prospectively evaluate the improvement in working and declarative memory,
two cognitive prefrontal- and hippocampus-dependent processes, respectively, and the effects
of tianeptine on serum BDNF levels.
One of the main challenges in the treatment of Bipolar Disorder (BD) is to achieve better
functioning outcomes after syndromal recovery. Available treatments are reasonably effective
in reducing acute symptoms, but many times the syndromal recovery is not accompanied by the
restoration of functioning capabilities. This is particularly true for bipolar depression,
which is responsible for most of the burden associated with BD. Even treatment-responsive
patients, who remain symptomatically well for extended periods of time, frequently
demonstrate sub-threshold symptoms and continuing psychosocial morbidity and cognitive
impairment. The cognitive impairment that persists during interepisode periods stands out as
a major correlate of functional impairment, and may be a core aspect of the BD
pathophysiology. Beyond that, cognitive impairment worsens with cumulative episodes.
Functional and morphometric studies have shown changes in amygdala, hippocampus and
prefrontal cortex of patients with bipolar disorder. Effective treatments for bipolar
disorder, such as lithium and divalproex, have proved to prevent cellular atrophy, to have
antiapoptotic properties and to increase BDNF levels. Findings from neuropathological
studies have confirmed reduction and dysgenesis of neuronal cell lines in the hippocampus in
bipolar disorder. Ultimately, a main challenge in the treatment of BD is translating the
knowledge of neuronal plasticity and neurobiology of the illness into novel therapeutic
options.
In this context, tianeptine stands out as a therapeutic agent with unique properties, which
match most of the conditions found in BD. The neurochemical properties of tianeptine vary
from those of other tricyclic and non-tricyclic antidepressants. Noteworthy, none of current
available medications for BD showed all these features: 1) tianeptine exert opposite effects
than chronic stress in neurons, increasing neuroprotective factors what may help to quench
the cycle of affective episode recurrence and neural and deterioration; 2) tianeptine
affects neuroplasticity in the hippocampus and have been reported to increase dendritic
lengths; 3) tianeptine increases BDNF levels in the amygdala; 4) tianeptine attenuated
stress-induced glutamate release in amygdala; 5) tianeptine has anticonvulsant properties
via adenosinergic A1 receptors; 6) tianeptine has analgesic effects.
In the present research project, we plan on conducting an enriched maintenance study of the
use of tianeptine as an adjunctive therapy in bipolar depression. All participants will
receive tianeptine in an open label manner for a period of two months, following which they
will be assigned randomly to the treatment with tianeptine or placebo in a double-blind
fashion for six months. All patients will remain on treatment as usual for the duration of
the trial. This trial will allow the investigation of the efficacy and tolerability of
tianeptine 37.5mg/day as an adjunctive treatment of bipolar depression and its impact on
clinical variables associated with the aftermath of a bipolar depression episode.
Considering that tianeptine is approved to be used orally in humans and has been on the
market for depression, a low risk intervention using a novel approach may be provided by
this clinical trial. Along with clinical response, we will prospectively evaluate the
improvement in working and declarative memory, two cognitive prefrontal- and
hippocampus-dependent processes, respectively, and the effects of tianeptine on serum BDNF
levels.
;
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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