Since data from the same group indicated that stopping medications was the primary reason for symptomatic relapse,37 strategies to enhance the level of medication adherence are also a critical component for achieving remission and Gamma-secretase inhibitor recovery. Time course of antipsychotic effect If all of the above
considerations are addressed, one Inhibitors,research,lifescience,medical of the most challenging issues remains whether or not the patient has had an “adequate” trial. The response to medications varies considerably between patients. When we asked experts38 how long an adequate initial trial should last, the responses ranged from 2.6 to 5.5 weeks. Textbooks of psychiatry had generally stated that response might be delayed for weeks rather than days.39 Recent meta-analyses have challenged that assumption. Agid et al40 evaluated 42 studies including 7450 patients Inhibitors,research,lifescience,medical and found that the greatest proportion of improvement in psychotic signs and symptoms (even controlling for placebo response) in short-term trials occurred in the
first week. Leucht et al41 replicated these results utilizing individual patient data. In addition, when examining data available in a subset of patients at 1 year, they found that most of the drug Inhibitors,research,lifescience,medical effect observed at 1 year had already occurred by week 4. Subsequent post-hoc analyses42 found significant separation between drug and placebo effects on positive psychotic symptoms even after only 24 hours. These data have reinvigorated the effort to use early response/nonresponse as a predictor of subsequent response.43,44 Correll et al45 were the first to attempt to predict nonresponse at 4 weeks using the change Inhibitors,research,lifescience,medical of symptoms at 1 week in a sensitivity-specificity analysis in 131 patients receiving uniform treatment with fluphenazine. When Leucht et al46 conducted a receiver-operator analysis to answer this question, a response of less than 20% improvement on the total Brief Psychiatric Rating Scale47 (BPRS) best predicted nonresponse at 4 weeks. Chang et al48 reported similar results in 123 patients treated with risperidone, Inhibitors,research,lifescience,medical and Leucht et al49 replicated
their earlier findings in 1996 patients from pooled olanzapine clinical trials. Kinon et al50 and Ascher-Svanum et al51 reported on post-hoc analyses of 1077 Montelukast Sodium patients who had participated in a series of double-blind trials involving olanzapine and found that a less than 20% reduction in PANSS scores at 2 weeks was associated with good predictive power to identify patients unlikely to respond by 12 weeks. Patients with poor early response were also found to be more likely to discontinue from the trial and their cost of care was significantly higher than those with more robust early response.51 Kinon et al52 conducted a prospective study of 630 patients treated with risperidone (2 to 6 mg/day).