Schizophrenia Clinical Trial
Official title:
L-Carnosine, an Antioxidant and AGE Inhibitor (Advanced Glycation End Products) for Cognitive Enhancement Among Persons With Schizophrenia: A Randomized, Add-on Double-Blind, Placebo Controlled, Clinical Trial
The investigators' hypothesis is that oral L-carnosine treatment (as compared with placebo)
will enhance cognitive abilities (specifically: measures of attention, executive function,
working memory, visuospatial ability and language) in persons with schizophrenia or
schizoaffective disorder. Secondarily, they hypothesize that there will be secondary
improvements in positive, negative and mood symptoms with L-carnosine treatment.
The investigators aim to test these hypotheses by conducting a randomized, placebo
controlled, add-on treatment trial of L-carnosine (added to existing antipsychotic
treatment) up to 84 recruited subjects with Diagnostic and Statistical Manual of Mental
Disorders, 4th Edition, Text Revision (DSM-IV-TR) schizophrenia/schizoaffective disorder for
a period of 16 weeks. Measures of cognition and psychopathology will be utilized for
evaluating primary and secondary outcomes, along with safety assessments.
OBJECTIVE:
Based on the available neuroscience and human data, we hypothesize that supplemental
L-carnosine treatment (a potent naturally occuring antioxidant and anti-glycation agent)
will be a useful disease modifying agent when used adjunctively with antipsychotic drugs in
patients with a diagnosis of either schizophrenia or schizoaffective disorder. More
specifically, our hypothesis is that oral L-carnosine treatment (as compared with placebo)
will enhance cognitive abilities (specifically: measures of attention, executive function,
working memory, visuospatial ability and language) in persons with schizophrenia or
schizoaffective disorder. Secondarily, we hypothesize there will be secondary improvements
in positive, negative and mood symptoms with L-carnosine treatment.
RESEARCH PLAN:
A randomized, placebo controlled, add-on treatment trial of L-carnosine (added to existing
antipsychotic treatment) for a period of 16 weeks. Measures of cognition, and
psychopathology will be utilized for evaluating primary and secondary outcomes, along with
safety assessments.
METHODS:
Up to eighty-four subjects with DSM-IV-TR schizophrenia/schizoaffective disorder will be
recruited from Western Psychiatric Institute and Clinic, Mayview State Hospital, Mon Yough
Community Services, Inc. and Dubois Regional Medical Center using a 1:1 randomization,
subjects who sign a informed consent document will be randomized to receive L-carnosine or
placebo. During a 4 week titration period, the L-carnosine dosage will be increased from 500
to 2000 mg/day, and continued for an additional 8 weeks. If side-effects are noted, a
minimum of 500 mg/day of L-carnosine can be used.
A computerized cognitive battery will form the main efficacy measures and be administered at
baseline and at visit 6 (i.e. just prior to the 4 week taper); some of these measures will
be administered at visit 4 (28 days). Standard psychopathology rating scales will be
administered to evaluate secondary aims such as impact on positive and negative symptoms of
schizophrenia. Safety will be assessed by tailing a careful medical history and physical
examination at screening and evaluating results of laboratory measures. Any adverse effects
will be assessed by asking questions at each visit, and if required bringing subjects in for
assessments outside the scheduled visits.
SIGNIFICANCE:
Cognitive dysfunction in persons with schizophrenia is a serious limitation to achieving
significantly better functional outcomes (Green, et. al., 1996). Till recently, therapeutic
nihilism prevailed when it came to treatments that improve cognitive abilities in
schizophrenia. One reason for this pessimistic view was that cognitive dysfunction was not
considered to be malleable to treatment but instead was thought to represent an unchanging
dimension of the illness. However, that view is now changing, and psychosocial and cognitive
remediation techniques are being evaluated to treat cognitive dysfunction in schizophrenia.
A recent synthesis of data would suggest that mediators of a better cognitive outcome may
also include agents that target the inefficient antioxidant defenses in persons with
schizophrenia, or those that counter NMDA-glutamate neuronal excitotoxicity (Yao et al.,
2001). These mechanisms may underlie the neuronal membrane pathology in schizophrenia, and
in turn these abnormalities may contribute to the cognitive dysfunction and decline reported
during the course of the illness. The benefits of L-carnosine (a naturally occurring
antioxidant and anti-glycation agent) for improved cognitive abilities and in social
behavior and communicative skills were reported in a random-assignment, double-blind,
placebo-controlled trial in children and adolescents with autism; specifically improvements
in receptive language scores and socialization and communication skill scores (Chez et al.,
2002a).
The primary focus of this study is to evaluate the ability of L-carnosine, a naturally
occurring dipeptide, to enhance cognitive abilities in people with schizophrenia. The study
will also evaluate whether L-carnosine has secondary benefits for positive and negative and
mood symptoms. As a relatively benign agent, L-carnosine offers the potential to achieve a
significant clinical impact in improving cognitive dysfunction in persons with
schizophrenia, if efficacy is confirmed.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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