Evidence-Based Reviews

Which antipsychotic do I choose next?

Current Psychiatry. 2006 September;5(9):27-43

CATIE phases 1 and 2 provide a compelling rationale for individualized treatment, which should be standard clinical practice for schizophrenia.

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References

1. Stroup TS, Lieberman JA, McEvoy JP, et al for the CATIE investigators. Effectiveness of olanzapine, quetiapine, risperidone, and ziprasidone in patients with chronic schizophrenia following discontinuation of a previous atypical antipsychotic. Am J Psychiatry 2006;163:611-22.

2. McEvoy JP, Lieberman JA, Stroup TS, et al for the CATIE investigators. Effectiveness of clozapine versus olanzapine, quetiapine, and risperidone in patients with chronic schizophrenia who did not respond to prior atypical antipsychotic treatment. Am J Psychiatry 2006;163:600-10.

3. Lieberman JA, Stroup TS, McEvoy JP, et al. Effectiveness of antipsychotic drugs in patients with chronic schizophrenia. N Engl J Med 2005;353:1209-23.

4. Nasrallah HA. CATIE’s surprises: In antipsychotics’ square-off, were there winners or losers? Current Psychiatry 2006;5(2):52-65.

5. Buckley PF. Dosing equivalency of second-generation antipsychotics. J Clin Psychopharmacol 2005;25(5):501-2.

6. Davis JM. The choice of drugs for schizophrenia. N Engl J Med 2006;354(5):518-20.

7. Citrome L, Stroup TS. Schizophrenia clinical antipsychotic trials intervention effectiveness and number needed to treat: How can CATIE inform clinicians? Int J Clin Pract 2006 (in press).

8. Ragins M. Should the CATIE study be a wake-up call? Psychiatr Serv 2005;56:1489.-

9. Lieberman JA, Hsiao J. Interpreting the results of the CATIE study. Psychiatr Serv 2006;57:139.-

CATIE phase 2 offers insights on efficacy an tolerability

After nearly 3 out of 4 phase 1 patients stopped taking their assigned antipsychotics within 18 months, researchers in the Clinical Antipsychotic Trials of Intervention Effectiveness (CATIE) braced themselves for phase 2.^{February 2006)}

CATIE’s eligibility criteria are broad and include schizophrenia patients with comorbid conditions such as substance abuse and mood disorders. The primary outcome measure is all-cause treatment discontinuation, which incorporates efficacy, safety, tolerability, patient choice, and clinician choice (Table 1).

Phase 1 compared the efficacy and safety of four second-generation antipsychotics (SGA) and one first-generation antipsychotic (FGA).³ Nasrallah concluded that—despite the high discontinuation rate in that phase—there were “no winners or losers” among the five antipsychotics. The results, Nasrallah concluded:

provide a compelling rationale for clinicians to match medication profiles to individual patients
support the need for clinicians to have choices among medications when treating patients with schizophrenia.⁴

Table 1

Drug discontinuation patterns in CATIE phase 1

Measures	Findings after 18 months
% of patients who discontinued medication for any reason	Olanzapine (64%)	Ziprasidone (79%)
	Risperidone (74%)	Quetiapine (82%)
	Perphenazine (75%)
Time to discontinuation for any reason	Longest (most favorable) with olanzapine, but not statistically longer with olanzapine than with ziprasidone or perphenazine
	No statistical difference among risperidone, quetiapine, ziprasidone, and perphenazine
Time to discontinuation for lack of efficacy*	Longer with olanzapine; no statistical difference among risperidone, quetiapine, ziprasidone, and perphenazine
Time to discontinuation for intolerable side effects	No statistical difference among agents
Rate of discontinuation for intolerable side effects	Highest (19%) with olanzapine (primarily because of weight gain or metabolic effects with this medication)
Rate of discontinuation for extrapyramidal effects	Highest (8%) with perphenazine
Rate of discontinuation for intolerability (overall)	Lowest with risperidone (10%)
* Nonequivalent dosing in CATIE phase 1 is an ongoing debate.

What to do next?

When an initial antipsychotic proves inadequate or causes intolerable side effects, how do you choose a more efficacious or tolerable medication? Phase 2 offered CATIE patients and their clinicians two choices—an efficacy and a tolerability pathway (Figure).^1,2

CATIE phase 2: Distribution of patients in efficacy and tolerability pathways

Efficacy pathway. Patients who chose the efficacy pathway were randomly assigned to clozapine (50%) or olanzapine, risperidone, or quetiapine.¹ Researchers selected clozapine as the major efficacy comparator because of its robust effects in treatment-refractory schizophrenia. Clozapine was given open-label because of its safety monitoring requirements; other treatments were double-blind.

As in phase 1, the primary outcome measure was time until discontinuation for any reason. Secondary outcome measures included time to discontinuation because of side effects, patient choice, or lack of efficacy.

Tolerability pathway. Patients who chose the tolerability pathway were randomly assigned to double-blind treatment with ziprasidone, olanzapine, risperidone, or quetiapine.² Ziprasidone was the major comparator because of clinical data showing a favorable tolerability profile.

The primary outcome measure was time to discontinuation for any reason. Secondary outcomes included reason for discontinuation (as determined by the study clinician), symptomatic ratings, and evaluations of adverse effects.

Trial duration. No patients in either pathway received the same antipsychotics they had taken in phase 1. All patients could continue treatment through the 18 months of the CATIE trial or until they completed 6 months in phase 2.

Efficacy pathway results

Discontinuation. Consistent with literature about its efficacy in treatment-refractory schizophrenia, clozapine showed a robust clinical effect. Overall, more patients receiving clozapine stayed on treatment and for longer periods, compared with patients receiving olanzapine, risperidone, or quetiapine (Table 2).

On secondary measures, discontinuation for lack of efficacy was significantly lower with clozapine (11%) than with:

olanzapine (35%)
risperidone or quetiapine (each at 43%).

Discontinuation rates because of adverse effects or by patient choice were the same across all medications (Table 3). Patients on clozapine achieved better ratings in overall psychotic symptoms, positive symptoms, and general function, but not in negative symptoms.

Weight gain. On average, patients gained more weight while taking olanzapine (+1.1 lb/mo) than with:

risperidone (+0.5 lb/mo)
clozapine (+0.5 lb/mo)
quetiapine (+0.5 lb/mo)

Differences in weight gain—or in metabolic parameters or other adverse effects—were not statistically significant, however.

Table 2

Phase 2 efficacy pathway: Discontinuation for any reason

Measure	Clozapine	Olanzapine	Risperidone	Quetiapine
How many patients discontinued	25 of 49 (56%)	12 of 19 (71%)	12 of 16 (86%)	13 of 15 (93%)
Median time to discontinuation	10.5 months	2.7 months	2.8 months	3.3 months

Table 3

Reasons patients stopped taking their medications in CATIE phase 2

Reason	Efficacy pathway	Tolerability pathway
All cause	69%	74%
Lack of efficacy	26%	29%
Lack of tolerability	10%	15%
Patient choice	26%	24%

Tolerability pathway results

Discontinuation. Patients in the tolerability pathway took olanzapine or risperidone significantly longer—median 6.3 and 7 months, respectively— compared with ziprasidone (4 months) or quetiapine (2.8 months).

Time to discontinuation during phase 2 was the same across all drugs among patients who entered phase 2 because of intolerable side effects in phase 1.
Time to discontinuation because of side effects also was similar whether patients discontinued phase 1 for lack of efficacy or intolerable side effects. Patients stopped treatment in the efficacy and tolerability pathways for similar reasons (Table 3).

Which antipsychotic do I choose next?

References

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