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KMID : 0361520050160020109
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Korean Journal of Psychopharmacology
2005 Volume.16 No. 2 p.109 ~ p.120
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Effectiveness and Tolerability of Long-Acting Risperidone£ºA 12 Weeks, Multi-center Switching Study from Oral Antipsychotics
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Á¶¼ºÁø/±èÂùÇü/¹Ú¿ø¸í/À±Áø»ó/Á¤Àοø/ÀÌ»ó¿/À̾çÇö/È«°æ¼ö/±è´ëÈ£/±è¿µÈÆ
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Abstract
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Objective£ºTo evaluate maintained effectiveness and tolerability when treated with long-acting risperidone compared to the previous antipsychotics in patients with schizophrenia or other psychotic disorders and to compare maintained effectiveness between oral risperidone and non-risperidone subgroups.
Methods£ºSubjects aged at least 18 years who required long-term antipsychotic therapy and who have been symptomatically stable on a stable dose of antipsychotics during the last month were enrolled in the non-randomized, single-arm, multi-center, 12 weeks duration study. Antipsychotic medications were switched from oral antipsychotics to long-acting risperidone. Injections were administered every 2 weeks. Most patients were started on 25mg long-acting risperidone injection or 37.5mg in some patients. The dosage were adjusted according to the patients¢¥ symptoms and responses to treatment at the discretion of investigators. Oral antipsychotics were continued at the same dose as before for 2 weeks and then were stopped or tapered off within next 7days.
Results£ºA total of 204 patients with schizophernia (N=192) and other psychotic disorder (N=12) from 20 sites in Korea were enrolled. The drop-out rate was 22.5% at 12 weeks. LOCF analysis has been performed. At 12 weeks after switching from oral antipsychotics to long-acting risperidone, statistically significant improvement was observed from baseline across all symptom domains including PANSS total, positive, negative, general subscale, CGI-S(Clinical Global Impression-Severity) scores and GAF(Global Assessment of Functioning) scores. The proportion of responders was 36.8% where response was defined as ¡Ã20% reduction from baseline PANSS total score. The proportion of symptom worsening at 12 weeks was 7.4%(N=15) where symptom worsening was defined as ¡Ã20% increase from baseline in PANSS total score or drop-out due to insufficient response or any 2 points change on any of 4 PANSS psychotic items(delusion, conceptual disorganization, hallucinatory behavior, suspiciousness/persecution) excluding changes in which the ratings remained at nonpsychotic levels (i.e £¾3). Significant improvement from baseline was also observed in the measure of parkinsonism assessed using Extrapyramidal Symptom Rating Scale (ESRS). In addition, overall, patients were satisfied with long-acting risperidone injection on a single item measure of satisfaction. When subgroup analysis was performed on the basis of previous antipsychotics before switching to long-acting risperidone, no statistically significant differences were detected between oral risperidone(N=139) and non-risperidone subgroup(N=65) on all measures of effectiveness and tolerability including baseline demographic and clinical characteristics, symptom improvements, proportion of symptom improvement or worsening and ESRS score changes.
Conclusion£ºOur study results demonstrated maintained effectiveness and tolerability of long-acting risperidone microsphere and also could confirm successful switching from not only oral risperidone but also non-risperidone to long-acting risperidone injection.
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