Schizophrenia Clinical Trial
Official title:
The Use of Oxytocin as Adjunctive Therapy for the Treatment of Schizophrenia: a Randomized, Double Blind Trial
Background: A large body of research has shown that Oxytocin (OXT) is an important prosocial
peptide and there is also initial evidence that the central OXT system is altered in several
mental disorders that are characterized by severe social disturbances and deficits, such as
anxiety disorders with prominent social dysfunction (e.g., schizophrenia), mood disorders
and borderline personality disorder. OXT may reduce psychotic symptoms and may diminish
certain social cognition deficits that are not improved by current antipsychotic
medications.
Aims: The project has two main aims, listed below:
1. To assess the efficacy of intranasal OXT in reducing negative symptoms in patients with
schizophrenia in association with second-generation antipsychotics (SGA);
2. To use an Emotional Priming Paradigm task to assess pre- and post-treatment change in
the patients general cognitive and emotional status.
Study Design: Randomized, double-blind, placebo-controlled, cross over design. Materials and
methods: Patients involved in the study will be recruited in six centres in the north of
Italy. Each subject (aged 18-45, with a duration of the disorder no longer than 10 years)
will be enrolled after a screening phase. 80 patients will be randomly assigned to either 40
IU OXT once daily or vehicle placebo, in addition to their pre-study antipsychotic
medication regimen: all reasonable attempts maintain the same SGA dosages throughout the
study will be made. The study ratio is 1:1. The total study duration for each individual
subject will be approximately 8 months, which includes an up to 7-day screening period, a
baseline randomization visit, and a four month long cross-over treatment period. Subjects
will be trained by researchers about the self-administration of intranasal OXT. A
trustworthy caregiver will be trained as well. Each patient will receive every morning a SMS
text message on his mobile phone as a reminder for OXT administration.
Before starting the treatment, all patients will be assessed with standardized assessment
instruments and will undergo an in depth neuropsychological assessment; additional
evaluations, including safety evaluations, will be performed at 4 and 8 month follow-ups.
The primary outcome measure will be the negative score in the Positive and Negative Syndrome
Scale (PANSS) performed at 2,4,6 and 8 months since the start of the treatment.
The project has two main aims:
1. Aims of the cross-over study To assess the efficacy of intranasal OXT in reducing
negative symptoms in patients with SZ (as evaluated with PANSS), in association with
standard Second Generation Antipsychotics (SGA)treatment; recruited patients will be
aged 18-45 years and will have a disorder duration of no longer than 10 years.
2. Aims of the neuropsychological assessment To use an Emotional Priming Paradigm (EPP)
task to assess pre- and post-treatment change in the patients general cognitive and
emotional status.
The investigators aim at treating a large sample size of patients with schizophrenia,
consisting exclusively of patients with a limited disorder duration and rather young age,
for a sufficiently long period of time. Our rationale for employing a longer treatment
period than used in previous and on-going trials is to ascertain the possibility of a
positive OXT dose-response relationship, which would be observable, however, with longer
treatment exposure. Moreover, only patients with a disorder onset of 10 years or less will
be enrolled.
They will then be standardized in terms of AP treatment and randomized to OXT or placebo for
8 months.
OXT is a hormone that is naturally present in the human body, and recent studies have
suggested that patients with SZ show low levels of this neuropeptide. It is therefore
hypothesized that the treatment proposed in this project might balance apparently lower OXT
levels in these patients.
Finally, another innovative aspect of this project is the attention at ameliorating patients
adherence to treatment by supporting them with a reminder program (automatic SMS will be
sent every morning to remind patients the daily OXT self-administration) and involving a
trustworthy caregiver who will be trained in OXT administration and will be asked to monitor
the patient compliance by recording each self-administration on a written form.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Crossover Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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