Major Depressive Disorder Clinical Trial
Official title:
Efficacy Of Switching From SSRI to Desvenlafaxine on Cognitive Function In Patients With an Acute Episode of Major Depression
Given the importance of cognitive function on depressed patients' treatment outcome and
return to premorbid functioning, the effect of antidepressant drugs on cognition has become
of primary concern. The aim of the present study is to assess the clinical outcome of
switching from a selective serotonin reuptake inhibitor (SSRI) to desvenlafaxine on cognitive
function in a Spanish sample of adults with moderate to severe major depressive disorder
(MDD).
This open-label clinical study will include a total of 36 MDD outpatients receiving treatment
with desvenlafaxine according to treating psychiatrist clinical judgment.
The primary efficacy endpoint will be changes from baseline to week 12 in cognitive function
measured by a composite z-score comprising the Digit Symbol Substitution Test (DSST) and Rey
Auditory Verbal Learning Test (RAVLT) scores. The secondary efficacy endpoints will involve
depression severity, additional measures of subjective and objective cognitive function
(including cold and hot cognitive function tasks), and functional status.
A matched sample of 36 healthy controls will be assessed in order to obtain reference data
for all cognitive function measurements. Patients with MDD and healthy controls will be
compared regarding cognitive function both at baseline and after 12 weeks.
BACKGROUND
Depression is a significant contributor to the global burden of disease and affects people in
all communities across the world. Today, depression is estimated to affect 350 million
people. The World Mental Health Survey conducted in 17 countries found that, on average,
about 1 in 20 people reported having an episode of depression in the previous year.
Depressive disorders often start at a young age; drastically reduce people's functioning and
often are recurring. For all these reasons, depression is the leading cause of disability
worldwide in terms of total years lost due to disability.
Commonly the diagnosis and treatment of major depressive disorder is based on mood symptoms.
However, cognitive impairments are often present in this disorder. In this respect, the
recent Diagnostic and Statistical Manual 5 (DSM-5) highlight impairment in cognitive function
as a criterion in the diagnosis of a major depressive episode (MDE) (American Psychiatric
Association. At clinical level, patients frequently present subjective complaints during and
after resolution of an MDE. Moreover, objective deficits measured by neuropsychological tests
are also reported in different cognitive domains in cold cognitive function - executive
function, processing speed, attention, learning or memory- (Hammar &Ardal, 2009) or also in
hot cognitive function -negative biases in perception, attention and memory, and aberrant
reward/punishment processing-.
Different meta-analyses have demonstrated that these deficits may emerge from the first
depressive episode with relevant intensification during each acute MDE persisting in some
depressive patients even during the resolution of the acute episode. These deficits, both in
an acute episode and in remission, have a relevant impact on clinical and functional
outcomes, in the first case by reducing the chance to fully recover and in the second by
increasing the risk of relapse. Moreover, cognitive deficits have shown to have a negative
influence in functional performance in academic, social and working life (Lee et al., 2013,).
In this context, recent studies have shown that a larger number of MDD episodes, a longer
duration of illness and a poor response to antidepressant treatments might explain the
maintenance of cognitive dysfunction, even in patients with some clinical response.
Persistent cognitive deficits in depression play a crucial role in some patients׳ ability to
achieve a functional recovery. With this respect, cognitive function in depression is
significantly also related to employment status. A preliminary study suggests that deficits
in executive functioning have a mediating effect on the relationship between depression and
impaired activities of daily living. Moreover, mood disorder patients with neuropsychological
deficits tend to be less compliant with antidepressant treatment (Martinez-Aran et al., 2009)
and show an increased risk for suicide. In this context, the identification and treatment of
specific cognitive deficits may be a cardinal aspect in the achievement of depression
recovery and, even more important, in the functional normalization of patients to their
pre-morbid levels.
At present there is a growing interest on the role of antidepressant treatment in the
modulation of cognitive deficits associated with depression. Despite the wide array of
effective antidepressant agents, the knowledge on the impact of available drugs on cognitive
function constitutes a relevant unmet need. Indeed, the number of studies focusing on this
issue is relatively scarce and the outcome of cognitive symptoms is widely variable.
Potential pro-cognitive effect of a particular antidepressant mostly relay on its specific
mechanisms of action, anf in the last years the evidence accumulated have support that drug
involving more targets such as dual (duloxetine) or multimodal (vortioxetine) antidepressants
show more pro-cognitive properties than those with one major mechanism (SSRI).
However, the clinical studies putting cognitive dysfunction as the primary outcome in
depression trials are scarce and further support of these initial promising findings of the
effects of dual/multimodal antidepressants on cognition are required.
OBJECTIVES
This open-label clinical study will evaluate the clinical outcome of switching to
desvenlafaxine on cognitive function of patients with major depressive disorder with
inadequate response to selective serotonin reuptake inhibitor (SSRI)
* Primary Objective
To study differences in cognitive function in moderate to severe MDD patients with inadequate
response to SSRI and healthy controls at baseline and after 12 weeks of treatment with
desvenlafaxine.
* Secondary Objective
To study differences in subjective cognitive function (cognitive complains), measured by
PDQ-5 at baseline and after 12 weeks of treatment with Desvenlafaxine.
To study differences in cognitive function, measured by neuropsychological tests battery
(including cold and hot cognitive function) at baseline and after 12 weeks of treatment with
desvenlafaxine.
To study differences in depression severity, measured HDRS-17 and CGI at baseline and after
12 weeks of treatment with desvenlafaxine.
To study changes in subjective remission and functional status measured with Remission
Depression Questionnaire (RDQ) and the Short Assessement Functioning Test (FAST),
respectively.
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