Schizophrenia Clinical Trial
Official title:
Investigation of Body Mass Index, Body Composition, Resting Energy Expenditure, Respiratory Quotient and Metabolic Changes Following a Switch From Olanzapine, Quetiapine or Risperidone to Aripiprazole
Weight gain is a serious, common side effect of many antipsychotic medications. On average,
the highest amounts of weight gain are found to occur in people taking clozaril and
olanzapine, but with significant weight gain occuring in those on the other atypical
antipsychotics as well.
We, the researchers at the University of North Carolina, propose an open-label
observational, pilot study of the changes in weight, BMI, body composition, and lipids,
glucose, insulin and other metabolic parameters occurring in subjects as they switch from
treatment with olanzapine, risperidone or quetiapine to aripiprazole. This medication switch
will be determined prior to their entering this study by their treating psychiatrist. We
also will determine resting energy expenditure (REE) and respiratory quotient (RQ) as
measured by metabolic cart to determine if either energy expenditure or the propensity to
store energy as fat may be involved in any changes to weight that are detected. Food intake,
hunger, and physical activity will also be assessed.
Weight gain is a serious, common side effect of many antipsychotic medications. It is a
frequent cause of poor adherence to antipsychotic medications and a major contributor to
medical problems including Syndrome X, various cancers, osteoarthritis and sleep apnea.
Syndrome X, also called the Metabolic Syndrome, is a constellation of abnormalities of
metabolism that confer a high risk of coronary heart disease. Syndrome X includes glucose
intolerance, dyslipidemia, hypertension, and central obesity. Long-term patients on
antipsychotic medications have markedly increased rates of Syndrome X that are consistent
with increased cardiovascular morbidity and decreased life expectancy.
A recent meta-analysis estimated weight gain at 10 weeks of treatment for a variety of
antipsychotics and found that clozapine had the highest average weight gain (4.45 kg),
followed by olanzapine (4.15 kg), quetiapine (2.2 kg), risperidone (2.18 kg), and
ziprasidone (0.04 kg) . For some drugs weight gain continues over many months, with the time
to plateau being directly related to the initial degree of weight gain. Early data for the
most recently approved antipsychotic, aripiprazole, shows it to be weight neutral but the
characteristics of its effects on weight are still to be determined. A recent publication of
224 subjects switching by three different switching strategies from haloperidol,
thioridazine, risperidone or olanzapine to aripiprazole found weight loss of between 1.3 and
1.7 kg after 8 weeks on aripiprazole. Cholesterol levels improved in subjects switching from
olanzapine to aripiprazole.
Atypical antipsychotic medications that can improve the factors associated with Syndrome X
could offer a very attractive alternative for patients who have already developed this
constellation of symptoms during treatment with other antipsychotics. It is not known if a
switch to aripiprazole from an atypical antipsychotic medication that has caused excessive
weight gain and/or abnormalities of glucose, lipids or blood pressure will result in
significant improvement in these factors or simply halt worsening. If worsening is only
halted, then switch from a weight-inducing drug to aripiprazole should be done early. If
factors associated with Syndrome X can be reversed, then switch to aripiprazole would be
very beneficial even after abnormalities have developed.
We propose an open-label pilot study of the changes in weight, BMI, body composition, and
lipids, glucose, insulin and other metabolic parameters occurring in subjects as they switch
from treatment with olanzapine, risperidone or quetiapine to aripiprazole. We also will
determine resting energy expenditure (REE) and respiratory quotient (RQ) as measured by
metabolic cart to determine if either energy expenditure or the propensity to store energy
as fat may be involved in any changes to weight that are detected. Food intake, hunger, and
physical activity will also be assessed.
Recruited subjects will enter a screening phase where patient eligibility is determined
through assessments of psychiatric and physical health, including physical examination,
blood tests and urine drug screen. Subjects not meeting eligibility criteria will be
discontinued.
Thirty subjects will be enrolled into this open label study. At entry into the study,
anthropometric measures (wt, ht, waist, hip), body composition, respiratory quotient (RQ),
resting energy expenditure (REE), and measures of food intake, hunger, and physical activity
will be assessed. Additionally, the Positive and Negative Symptom Scale (PANSS) will be used
to assess clinical status and all women will have a blood pregnancy test as required prior
to having a DXA scan. Following completion of these assessments, subjects will begin a two
week cross-taper from their current antipsychotic to aripiprazole. Psychiatric symptoms,
weight, medical status and medication query will be reassessed after 2, 4, 8 and 12 weeks.
RQ and hunger will be reassessed at the 4 week time point. Fasting bloodwork, pregnancy
test, urine drug screen, vital signs, and all baseline assessments will be repeated at the
12 week time point or at early termination. During the study, dosage of aripiprazole will be
tailored to each subject's need based on symptoms and side effects, and will remain at or
below the maximum recommended dosage.
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