Schizophrenia Clinical Trial
Official title:
A Double-Blind, Placebo-Controlled Trial of Reward Responsivity During Nicotine Withdrawal in Smokers With Schizophrenia and Normal Controls
It has been suggested that patients with schizophrenia smoke in order to produce amelioration of dysfunctional dopaminergic pathways allowing them to experience pleasure and satisfaction and overcome anhedonia. No studies have assessed the effects of nicotine withdrawal on reward responsivity in patients with schizophrenia. The investigators believe that an understanding of this is crucial if improved treatments for nicotine dependence are to be developed for this patient population. If this group already has deficits in reward responsivity as a symptom of the disease then they may be particularly prone to the effects of nicotine withdrawal on reward systems. Smoking cessation may lead to a further decrease in their responsivity to pleasurable stimuli and worsening anhedonia. Treatments for smoking cessation may need to ameliorate any increased deficits if they are likely to be effective in patients with schizophrenia.
Heavy smoking continues to represent a significant public health problem for people in the
general population and for people with major mental illness. Twenty-four percent of adults
in the general population smoke and it has been estimated that 74-92% of people with
schizophrenia smoke. While effective treatments for smoking cessation have been developed,
response rates are modest and relapse rates are high. Approximately 70% of people who quit
smoking with effective treatments relapse to smoking within one year. A syndrome of negative
affect and anhedonia has been described as an important component in maintenance of
dependence on nicotine. It has also been suggested that preventing the syndrome of anhedonia
and negative affect during early abstinence may reduce relapse rates. If the syndrome of
anhedonia can be measured objectively and quantitatively, we will be better able to test
treatments for this withdrawal syndrome. It is our hypothesis that the syndrome of anhedonia
during early abstinence from nicotine is quantifiable as a deficit in reward responsivity.
Animal studies suggest that nicotine withdrawal is associated with an alteration in reward
responsivity. Brain stimulation reward thresholds have been used to measure anhedonia and
responsivity to reward in animal models. Nicotine withdrawal has been associated with a
significant decrease in brain reward function as measured by elevations in brain reward
thresholds that persist for 4 days. Nicotine withdrawal has also been associated with
failure of conditioning to an environment paired with novel stimuli, possibly due to a
decrease in reward associated with novel stimuli. Drug withdrawal states have also been
associated with inhibition of mesolimbic release in murine models.
We propose a randomized placebo controlled trial to investigate the effects of nicotine
abstinence on reward responsivity in patients with no major mental illness and in patients
with schizophrenia.
Principal Aims:
Aim 1: To evaluate the effects of nicotine withdrawal on a measure of reward responsivity
Hypothesis 1a: Normal controls and subjects with schizophrenia will demonstrate
deterioration on a measure of reward responsivity during abstinence (placebo condition)
compared to baseline. (Primary Outcome Measure)
Aim 2: To evaluate the effects of transdermal nicotine on reward responsivity during
abstinence.
Hypothesis 2a: Normal controls and subjects with schizophrenia will demonstrate greater
response bias toward a rewarded condition following transdermal nicotine administration
relative to placebo patch during a 3 day period of abstinence.
Aim 3: To evaluate the effects of smoking abstinence and transdermal nicotine on a measure
of reward responsivity in patients with schizophrenia who smoke relative to normal control
smokers.
Hypothesis 3a: Subjects with schizophrenia will demonstrate decreased reward responsivity
during all conditions (baseline, nicotine replacement therapy condition and placebo
condition) relative to normal controls.
Secondary aims:
Aim 4: To evaluate the effects of nicotine withdrawal on cognitive function in smokers
Hypothesis 4a: Normal controls and subjects with schizophrenia will demonstrate poorer
performance on tests of cognition following placebo administration compared with baseline
and nicotine conditions.
We propose to test the effects of smoking abstinence and nicotine replacement therapy, using
nicotine transdermal patch on a measure of reward responsivity in patients who smoke. We
propose a randomized placebo controlled crossover trial with the primary outcome measure
being Response bias using a signal detection task.
Subjects are 70 patients with schizophrenia who smoke and 70 normal control smokers who do
not have a major mental illness and who are matched for age, sex and nicotine dependence.
Though we expect to consent 70 subjects in each group, we expect only 20 subjects in each
group to complete the study
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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