Schizophrenia Clinical Trial
Official title:
Social Cognition,Attentional Network and Nicotine Drug Dependency - A Pharmacological Clinical Trail
In the present study, we investigate healthy subjects and schizophrenic patients who frequently show very low attentional capacity with functional magnetic resonance imaging (fMRI) and electrophysiology (EEG) during attention-requiring tasks to assess the level of attentional network activity.
Nicotine is improving attentional capacity which goes along with an activation of the
attentional network in the brain. So far, however, it is unresolved whether nicotine is used
for the purpose of self-medication by those nicotine-dependent subjects who suffer from
subclinical or clinical attentional deficits which may sustain nicotine addiction. In the
present study, we investigate healthy subjects and schizophrenic patients who frequently
show very low attentional capacity with functional magnetic resonance imaging (fMRI) and
electrophysiology (EEG) during attention-requiring tasks to assess the level of attentional
network activity. It is anticipated that low attentional network activity (during baseline
condition, after nicotine challenge and after withdrawal) predicts the degree of nicotine
dependence including the strength of withdrawal symptoms and relapse rate after smoking
cessation. In addition, we expect that functional variations within alpha4beta2 nAch
receptor genotype are associated with attentional capacity and -by extension - with nicotine
dependence.
Additionally Self-medication of attentional deficits and of increased stress vulnerability
may contribute to nicotine-dependence both in schizophrenia patients and healthy subjects.
However, very little is known about the effect of nicotine on stress in schizophrenia. In
particular social stressors are highly relevant in schizophrenia often resulting in social
withdrawal. A factor contributing to the stress-eliciting nature of social interaction is
the misidentification of social information during communication with others. The present
project aims at an investigation of nicotine effects on such social information processing
and its neurophysiological correlates and on social stress responses. Using a 2x2-factorial
design effects of nicotine vs. placebo are experimentally investigated in smoking
schizophrenia patients in comparison to smoking healthy controls each after an overnight
smoking deprivation. Nicotine will be administered by nasal spray delivering a systemic does
of 2 mg nicotine. Event-related EEG potentials will be recorded during the presentation of
pictures of facial affect and neutral control stimuli to assess social information
processing and its neurophysiological correlates. In addition a videotaped semi-standardized
conversation skills role-play test will be used as a social stress situation to assess
self-reported and non-verbal affective responses.
;
Allocation: Randomized, Intervention Model: Factorial Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Basic Science
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