Schizophrenia Clinical Trial
Official title:
A Randomized Open-Label, Rater Blinded Assessment of Optimal Treatment Change Strategy to Risperidone for Patients Intolerant of Olanzapine
The purpose of this study is to compare three strategies for switching patients with schizophrenia or schizoaffective disorder to the atypical antipsychotic, risperdone, after they have been unsuccessfully treated with another atypical antipsychotic, olanzapine. In the second phase of this study, investigators will assess the effectiveness of behavioral therapy in reducing body weight in risperdone-treated patients who are overweight or have problems with diabetes or blood sugar.
Data regarding the safety and effectiveness of different strategies for switching subjects
with schizophrenia from one antipsychotic medication to another are very rare. Studies that
have examined various switching designs, especially with regard to the newer atypical
antipsychotic agents, suggest that either abrupt or gradual discontinuation does not
inevitably lead to worsening of symptoms. This study is randomized (patients are assigned
different treatments based on chance), open-label, with a parallel group design to assess
the safety and effectiveness of each of three strategies of discontinuing olanzapine and
starting risperidone. The first strategy is the discontinuation of olanzapine on the day
risperidone is started. The second strategy involves a reduction in the dose of olanzapine
to one half of the study entry dose on the day risperidone is started. The reduced dose of
olanzapine is to be given for one week and then discontinued. In the third strategy, the
dose of olanzapine remains unchanged for the first week, then is reduced by one half of the
study entry dose, and at the end of the second week is discontinued. In all three
strategies, patients take the same dose of risperidone: 1 mg by mouth twice a day for 3
days, then 2 mg twice a day for the next 4 days. Further increase or decrease of risperidone
dose and/or changing to a single daily dose can be carried out at the end of the first week.
Additionally, after 6 weeks of risperidone therapy, patients who are overweight or have
problems with diabetes or blood sugar may enter a second phase of the study that examines
weight loss. In this phase, patients are randomized to receive routine clinical care or
training on weight management behavioral techniques while continuing to take risperidone for
an additional 14 weeks. At the end of 14 weeks, total weight loss, changes in lipids,
cholesterol and other laboratory measures will be compared between the two groups. The study
hypothesis is that symptom improvement or worsening at week 14, as measured by total score
on the Positive and Negative Syndrome Scale (PANSS), should not differ depending on the
method of switching from olanzapine to risperidone. Safety evaluations incude collection of
adverse events, clinical laboratory tests and assessment of vital signs.
The patients will receive oral tablets of risperidone 1 to 2 milligram[mg] twice a day
(higher or lower dose and/or changing to single daily dose allowed at end of the first week)
for the duration of 6 weeks in phase 1, and then for 14 more weeks in phase 2 of the study.
Olanzapine: none; or half of the study entry dose for 1 week; or study entry dose for 1
week, then half of the study entry dose for an additional week.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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