Schizophrenia Clinical Trial
Official title:
Effects of Atomoxetine on Cognitive Function in Schizophrenia
The purpose of this study is to examine the effects of atomoxetine (Strattera™) on prefrontal cognitive functioning in persons with schizophrenia. Secondarily, the effects of atomoxetine on positive and negative symptoms and on cigarette smoking consumption in persons with schizophrenia will be examined.
Schizophrenia occurs in approximately 1% of the general population. Hallmark symptoms of
schizophrenia include positive and negative symptoms, as well as deficits in various aspects
of cognitive function, with particular reference to neuropsychological tasks related to the
prefrontal cortex (PFC). A leading theory with respect to these deficits in prefrontal
cortical functioning is that there is dysregulation (with overall hypofunction) of
mesocortical dopamine (DA) projections from the VTA to the prefrontal cortex (PFC) in
persons with schizophrenia, thus diminishing abilities on tasks mediated by these cortical
areas [1]. Further, it is thought that the high rates of smoking in schizophrenia (58-88%)
as compared to a non-psychiatric population (~25%) may be due in part to the tendency of
schizophrenic patients to remediate these neurocognitive deficits by cigarette smoking, as
nicotine has been shown to improve selected cognitive deficits in persons with this illness
[2-4], and in fact such cognitive deficits may be a vulnerability factor predisposing these
patients to initiate and maintain smoking [5].
Atomoxetine (Strattera™) which has efficacy in treating children and adults with Attention
Deficit Hyperactivity Disorder (ADHD). It increases extracellular levels of both NE and DA
in the PFC by blocking the NE transporter (NET), where it has been shown that DA is
predominately taken up non-selectively by NET [6]. In contrast, atomoxetine was not found to
increase extracellular DA in subcortical areas [6]. It can be theorized that atomoxetine may
selectively increase DA in the PFC (versus subcortical areas) by inhibition of NETs in the
PFC. Accordingly, since persons with schizophrenia are thought to have a deficit of DA in
the PFC, and excessive subcortical DA function, a NET inhibitor such as atomoxetine may
increase DA-dependent PFC-mediated neurocognitive functioning, and reduce negative symptoms
associated with this disorder, without worsening positive symptoms of schizophrenia.
Atomoxetine has been shown to be safe and effective for ADHD treatment in both children and
adults (Eiland, 2004). Little is known about Atomoxetine's effects in treating other
psychiatric disorders, however, it has been hypothesized that this medication may have
efficacy for cognitive remediation in the schizophrenic population (Friedman, 2004).
In order to more fully understand the effects of this medication, a double-blind,
placebo-controlled clinical trial is proposed in which sixty (60) participants with
schizophrenia who are cigarette smokers would be randomized in a double-blind manner to one
of three doses of atomoxetine [0.0 mg/day (n=20) , 40.0 mg/day (n=20), or 80.0 mg/day
(n=20)]. Doses were chosen in accordance with the FDA suggested dosing, including a schedule
of initiation starting with 40.0mg/day and a target recommended dose of 80.0mg/day which may
be reached within a three day period. The highest recommended dose is 100 mg/day. These
doses were ultimately selected for this study because they are doses that are believed to be
well-tolerated by patients, doses that may be achieved within the two-week period of this
study, and two doses that fit with our intention to study the dose-dependent effects of this
medication. Safety and effectiveness for these doses has been determined for patients 18
years of age and older with ADD, the population that has been studied using Atomoxetine.
Should we discover that our patients with schizophrenia do not tolerate these doses well
through extensive monitoring of their physiological and clinical symptoms, or that the
maximum dose of 80.0 mg/day cannot be reached during this time period, smaller doses will be
considered and the appropriate amendments will be submitted.
Participants would be assessed across three cognitive testing sessions over a two-week
period including baseline assessments Day 1 (prior to medication administration), on Day 8
(after one week of medication), and again on Day 15 (after two weeks of medication). No data
currently exists in the literature regarding specific improvements in neurocognitive
performance in schizophrenia with atomoxetine, although it has been hypothesized that this
medication may be specifically helpful in schizophrenia. Therefore we believe this will be
one of the first studies of its kind. We hypothesize that atomoxetine will dose-dependently
improve deficits in PFC-related cognitive performance in persons with schizophrenia. We
secondarily hypothesize that schizophrenic smokers will demonstrate a reduction in negative
symptoms and daily cigarette consumption with atomoxetine as compared to placebo.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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