Schizophrenia Clinical Trial
Official title:
Aspirin as Adjuvant Therapy in Young Psychotic Patients
In this double blind randomized clinical trial the investigators are going to exam influence of adjuvant Aspirin therapy on soft neurological signs (Heidelberg scale), positive and negative symptoms (PANSS), cytokine profile and inflammatory factors, as well as on cognition (MoCA) in young psychotic patients.
Schizophrenia as psychiatric paradigm is one of the most mysterious mental illness, for
decades remains a challenge to many clinicians and researchers with its complex, fundamental
mechanisms.
Soft neurological signs (SNS) are described as non-localized neurological abnormalities that
cannot be associated with damage of a specific brain region. It is believed that they are not
part of a well-defined neurological syndrome. They include neurological abnormalities with
deficits in sensory integration, motor coordination and sequencing of complex motor acts.
They have a higher prevalence in schizophrenic patients compared to healthy population.
Moreover, SNS have been consistently demonstrated in neuroleptic naive patients in the first
episode of illness. There is also an increased prevalence in non- schizophrenic relatives of
patients with schizophrenia. It is considered that they are not potentiated by
antipsychotics. For all these reasons it is believed that they are the inherent quality of
schizophrenia - "trait" marker, or endophenotypes.
According to the so-called "Two hit" hypothesis in the development of schizophrenia, there
are two periods of increased vulnerability. The first one is in a fetal age when it comes to
the interaction of genetic and environmental factors such as infection and inflammatory
processes who may also serve this function. The second period of vulnerability is a period of
adolescence, or early adult age when the influence of environmental factors leads to clinical
manifestations of the disease. It is thought that cytokines have key role in the first
strike.
Cytokines are mediators of communication between the neural elements in all aspects of the
development of the nervous system. Until now, numerous studies indicated modification of
specific cytokines in psychotic disorders and their possible role in the proposed concept of
"microglial hypothesis" of schizophrenia. Hypothesis of activation Th1 and Th2 immune
response, with a predominance of Th2 immune response is proposed in schizophrenia. Type-17
cytokines are important in mediating tissue damage in autoimmune diseases. Regulatory
cytokines suppress immune responses and maintain self-tolerance.
Consequently, the question is whether the combination of antipsychotic drugs with
anti-inflammatory drugs is more useful than independent antipsychotic therapy? Laan and
colleagues in 2010. carried out a randomized, double- blind, placebo - controlled study to
determine if the adjuvant aspirin therapy could be useful for patients who are already taking
antipsychotics. They concluded that the therapy antipsychotic + aspirin was significantly
superior to placebo + antipsychotic therapy. PANSS score was significantly lower in the
aspirin group.
The aim of the study would be to determine the effects of adjuvant aspirin therapy on Soft
Neurological Signs, PANSS and the cytokine profile. The investigators expect the reduction of
PANSS scores in both groups of patients (aspirin group and placebo group). If there is no
significant changes of SNS between groups, the results would support SNS as trait
characteristics of schizophrenia.
The research would be done on hospitalized patients at the Clinic for Psychiatric Disorders
"Dr Laza Lazarevic" in Belgrade. Part of the study (immunology) will be done on Medical
Faculty University of Kragujevac.
The study would be a randomized, double-blind, placebo controlled in two parallel groups of
50 to 60 patients who are neuroleptic naive or previously minimally medicated (in the past 6
months without any antipsychotic treatment) with the duration of the illness up to seven
years. The study would involve the patients of both sexes, aged 18 to 28 years, according to
ICD 10 criteria to satisfy diagnosis F 20 to F 29. Each patient who enters the hospital and
meets the inclusion criteria would be taken into consideration. If patient satisfies
exclusion criteria and sign consent, then s/he would be randomized into two groups:
Experimental group (antipsychotic + aspirin) and Control group (antipsychotic + placebo).
Patients in EG would receive 1,000 mg of aspirin pro die and pantoprazole 40 mg pro die in
two doses for gastric protection.
Only one researcher would know in which group patient belongs (would be responsible only for
randomization, would not be rater or treating psychiatrist). The same researcher would give
boxes with medications marked with the patient's name. In fact, all medications (aspirin,
pantoprazole, and placebo) would be packaged in the same looking capsules.
The protocol would consist of three planned visits for patients in both groups. On the first
visit blood samples would be taken for the implementation of immunological tests as well as
for laboratory inflammatory factors; patients would be subjected to clinical psychiatric and
physical examination, BMI measurement; PANSS scale will be done. After calming the signs of
acute psychosis, on 3rd day, patients would be examined with Heidelberg and MoCA scale;
patients would start to take Aspirin or Placebo. At the end of 6th week from the second visit
(+/- 3 days), on the third visit, blood samples would be taken again for analyzing cytokine
profile and inflammatory factors. PANSS, Heidelberg and MoCA scales would be performed again.
The investigators would consider the following factors: patient sex, age of the patients,
clinical characteristics, the role of heredity, type of therapy/ prescribed typical or
atypical antipsychotic; side effects of treatment and type of treatment response. Serum
concentrations of cytokines will be examined with commercial ELISA tests.
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