Schizophrenia Clinical Trial
Official title:
Randomized Controlled Trial of The Safety and Efficacy of Aripiprazole VS Ziprasidone in Schizophrenic Patients With Metabolic Syndrome and Diabetes Mellitus.
Introduction:
Schizophrenia is a serious mental illness. For majority of patients it is a lifetime
condition,characterized by intermittent episodes of hospitalization due to relapse or acute
symptom exacerbation. The nature and course of the disorder impose significant social and
economic burden. Relapse is costly, with hospitalization accounting for a substantial
portion of healthcare expenses. Second generation antipsychotic side effect such as
metabolic syndrome and diabetes mellitus will contribute additional costs to the treatment.
Many studies have since then provided convincing evidence for a high risk of diabetes and
other glucose abnormalities, metabolic syndrome and mortality due to elevated cardiovascular
risk in patients with schizophrenia.
However many studies has shown the effectiveness and safety of aripiprazole and
ziprazidone.In one of the study, aripiprazole showed improvement of negative schizophrenic
symptoms by 25% and 50% of functioning level from baseline. In term of safety,
antipsychotics considered to have a safer metabolic profile were amisulpride, ziprasidone
and aripiprazole.
Study objectives:
- To investigate the safety and efficacy of ziprazidone versus aripiprazole in the
treatment of schizophrenia patients with metabolic syndrome and diabetes mellitus.
- To investigate the reversibility of metabolic syndrome and diabetes parameters
following the treatment with ziprazidone versus aripiprazole.
Hypotheses:
* The proportion of reversibility of metabolic syndrome and diabetes parameters is higher
following the treatment of ziprazidone than aripiprazole.
Introduction:
Schizophrenia is a devastating mental illness that impairs mental and social functioning and
often leads to the development of comorbid diseases. Metabolic abnormalities have
historically been associated with illness such as schizophrenia. Many studies have since
then provided convincing evidence for a high risk of diabetes and other glucose
abnormalities, metabolic syndrome and mortality due to elevated cardiovascular risk in
patients with schizophrenia. These metabolic abnormalities are of major clinical concern not
only because of their direct somatic effects on morbidity and mortality but also because of
their association with psychiatric outcome, such as a higher prevalence of psychotic and
depressive symptoms, a lower functional outcome, a worse perceived physical health, and
lower adherence to medication.
Effective pharmacologic treatment of schizophrenia has been available since the 1950s. The
first-generation antipsychotics had an increased risk of extrapyramidal side effects, such
as dystonic reactions (example, fixed upper gaze, neck twisting, facial muscle spasms),
parkinsonian symptoms (example, rigidity, bradykinesia, shuffling gait, tremor), and
akathisia (example, inability to sit still, restlessness, tapping of feet).
The term "atypical antipsychotic" refers to newer antipsychotics that confer less risk of
extrapyramidal side effects than traditional antipsychotics. Although newer atypical
antipsychotics are associated with fewer neurologic side effects, they had a higher risk of
metabolic side effects such as diabetes, hypercholesterolemia, and weight gain. This effect
is independent from the development of diabetes; the exact mechanism by which atypical
agents might cause diabetes is unknown. Few drugs such as aripiprazole, sertindole,
amisulpride and ziprasidone were found to have promising effect in lowering metabolic
syndrome.
The study is designed to:
1. Identify safer treatment and high efficacy in schizophrenia. The efficacy of
ziprasidone in the treatment of schizophrenia has been demonstrated in both short-term
and long-term controlled trials. Ziprasidone has been shown to be comparable to
haloperidol, olanzapine and risperidone in alleviating overall psychopathology,
improving associated depressive symptoms and cognitive function in schizophrenia.
Ziprasidone was generally well tolerated in these trials, with a weight-neutral
profile, with limited discontinuations related to adverse events.
Ziprasidone has exhibited a low incidence of weight gain, and one analysis suggested it
carries a lower liability for weight gain than other atypical agents. In an open-label
study, patients whose medication was switched to ziprasidone from conventional
antipsychotics, risperidone, or olanzapine exhibited improvement in the lipid profile.
Ziprasidone has also demonstrated a low incidence of extrapyramidal symptoms and a low
risk of prolactin elevation. It has been associated with modest prolongation (<10
milliseconds) of the corrected QT(QTc) interval on electrocardiography(ECGs) obtained
during short-term, fixed-dose, placebo-controlled trials evaluating doses of up to 200
mg/day. A study evaluating QTc intervals at maximum steady-state plasma concentrations
demonstrated a 9-14-msec greater increase in QTc interval with ziprasidone than with
four other atypical antipsychotics, including olanzapine . The clinical relevance of
this magnitude of change is unclear. No excess risk of cardiac sequelae was observed in
the clinical development program (package insert for Geodon [ziprasidone], Pfizer Inc.,
New York, 2002).
Published data regarding the efficacy of aripiprazole in the treatment of schizophrenia
indicate superiority to placebo and comparability to risperidone, in Positive and
Negative Syndrome Scale (PANSS) total and Clinical Global Impression of Severity
(CGI-S) improvement scores. In these studies, aripiprazole demonstrated a favourable
safety and tolerability profile, with little propensity for weight gain or other
adverse metabolic effects.
2. Improving clinical practice This study will provide findings for the clinician to be
used later in the management of schizophrenia especially prognosis of the patient. The
aim is to achieve good outcome and minimising the side effects especially those causing
development of comorbidity.
Second-generation (atypical) antipsychotics have become first-line medications for the
treatment of schizophrenia and schizoaffective disorder, in large part due to their
consistently reduced association with movement disorders and comparable efficacy to
conventional agents. Direct comparisons among the atypical agents are, however, limited. In
contrast to earlier atypical antipsychotic agents, ziprasidone and aripiprazole share a
reduced propensity for weight gain and metabolic dysregulation. Given that obesity and
dyslipidemia are highly prevalent and probable contributors to the elevated rates of
morbidity and premature mortality among individuals with schizophrenia, these newer atypical
agents offer the potential for improved health outcomes in this population.
Obesity is a threat to health and longevity. Given that over one-third of the adults in the
United States are obese, practices causing major weight gain deserve careful consideration.
Obesity and weight gain have been associated with hypertension, type II diabetes, coronary
heart disease, stroke, gallbladder disease, osteoarthritis, sleep apnoea and respiratory
problems, and some types of cancer (endometrial, breast, prostate, and colon). Moreover,
obesity is a common concomitant of schizophrenia, and schizophrenic individuals appear to be
at increased risk for certain obesity-related conditions such as type II diabetes and
cardiovascular disease.
Weight gain may also cause patients taking antipsychotic medications to discontinue their
medications, which may predispose them to relapse. Historically, the extrapyramidal side
effects of antipsychotics outweighed any non-extrapyramidal side effects. With the advent of
newer "atypical" antipsychotics, extrapyramidal side effects are becoming less of a problem.
For other drugs, the degree of weight gain, estimated by the random effects regression at 10
weeks, ranged from 0.04 kg for ziprasidone (not significantly different from zero) to 4.45
kg for clozapine. Among the five new atypical antipsychotics in the study (ziprasidone,
risperidone, sertindole, olanzapine, and clozapine), ziprasidone had the lowest weight gain
(0.04 kg) and clozapine had the highest (4.45 kg).
This study will determine whether antipsychotic-associated metabolic syndrome and diabetes
mellitus can be reversed by switching to aripiprazole and ziprazidone. Currently there is no
data available on the above issue.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Outcomes Assessor), Primary Purpose: Treatment
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