Clinical Antipsychotic Trials of Intervention Effectiveness (CATIE) schizophrenia study (1,2,3)
double-blind, US study included a broad population of patients (n=1493) with chronic schizophrenia
minimal exclusion criteria and allowed co-existing conditions and use of other medications
publically funded
Phase 1
patients were randomly allocated to treatment with olanzapine, quetiapine, risperidone, ziprasidone (not available in the UK) or the typical antipsychotic, perphenazine for up to 18 months
doses were adjusted within a defined range according to clinical judgment
those receiving an atypical antipsychotic who discontinued treatment could be randomised to an alternative atypical antipsychotic in phase 2
Phase 2 had two arms:
A: ziprasidone vs. olanzapine, quetiapine, or risperidone; 2 or,
B: clozapine (open-label) vs. olanzapine, quetiapine, or risperidone
primary outcome in all phases was time to discontinuation for any reason - this endpoint reflects both clinician and patient judgements about efficacy and tolerability
Main Results
only 26% of patients (range 18–36%) completed the study on their first assigned antipsychotic in phase 1:
10–19% of patients discontinued treatment because of intolerable side effects
15–28% for lack of efficacy
24–34% discontinued first assigned antipsychotic for other reasons
time to discontinuation for any reason:
was significantly longer for olanzapine than for risperidone or quetiapine, but not for perphenazine or ziprasidone
in comparison with other treatments
olanzapine was associated with the lowest rate of discontinuations for efficacy reasons (15% vs. 24–28%)
however olanzapine was associated with the highest rate of discontinuations due to side effects (19% vs. 10–16%), notably weight gain or metabolic effects (9% vs. 1–4%, P<0.001)
more patients discontinued perphenazine due to extrapyramidal effects (8% vs. 2–4 %, P=0.002), and more patients discontinued quetiapine for anticholinergic side effects (31% vs. 20–25%, P<0.001)
in phase 2, many patients who discontinued their assigned atypical were able to successfully complete the study on an alternative
in phase 2A
the times to discontinuation for patients switched to risperidone or olanzapine were significantly longer than for those switched to quetiapine or ziprasidone
clozapine appeared more effective than the other atypical antipsychotics in phase 2B - this result should be judged however in the context of the low number of patients in this phase questions the validity of this finding
Conclusions
evidence from this study suggests that there is little to choose in terms of overall effectiveness between the antipsychotics studied, including the typical antipsychotic, perphenazine
all antipsychotics studied were associated with high rates of intolerable side effects and failure to control symptoms
for these patients with schizophrenia who prospectively failed to improve with an atypical antipsychotic, clozapine was more effective than switching to another newer atypical antipsychotic (3). However excluding clozapine (which requires careful safety monitoring), olanzapine appeared the most effective of the other atypical agents, although its benefits were limited by unacceptable weight gain and metabolic effects - however the olanzapine doses used were high (mean modal dose 20.1 mg) relative to the UK licensed dose range of 5–20mg daily, which may limit the relevance of these findings to UK clinical practice
"...The CATIE study clearly identifies the need for individualised antipsychotic treatment for patients with schizophrenia. Doctors and patients should carefully evaluate the tradeoffs between efficacy and side effects, to choose the antipsychotic (atypical or typical) that is most likely to be acceptable. No one antipsychotic is suitable for everyone (4)"
Reference:
Lieberman JA et al. New Engl J Med 2005;353:1209–23
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