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Clinical, Functional, and Economic Ramifications of Early Nonresponse to Antipsychotics in the Naturalistic Treatment of Schizophrenia

机译:精神分裂症自然治疗中早期对抗精神病药无反应的临床,功能和经济后果

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Objective: Early nonresponse to antipsychotics appears to predict subsequent nonresponse to treatment when assessed in randomized controlled trials of predominately acute inpatients treated for schizophrenia. This study assessed the predictive accuracy of early nonresponse to treatment and its clinical, functional, and economic ramifications in the naturalistic treatment of predominately chronic outpatients treated for schizophrenia. Methods: This post hoc analysis used data from a 1-year, randomized, open-label study of olanzapine, risperidone, and typical antipsychotics in the treatment of schizophrenia. If clinically warranted, patients could switch antipsychotics following 8 weeks of treatment. Patients completing 8 weeks of treatment (n = 443 of 664 enrollees) were included. Patients with early response (≥20% improvement from baseline on the Positive and Negative Syndrome Scale at 2 weeks) were compared with early nonresponders on symptom remission, functionality, perceptions of medication influence, and total health care costs at 8 weeks. Results: Early responseonresponse at 2 weeks predicted subsequent responseonresponse at 8 weeks with a high level of accuracy (72%) and specificity (89%). After 8 weeks, early nonresponders were less likely to achieve symptom remission (P < .001), improved less on functional domains (P < .05), perceived medication as less beneficial (P = .004), and incurred total heath care costs over twice that of early responders ($4349 vs $2102, P = .010). Conclusions: In the usual care of schizophrenia patients, early nonresponse appears to reliably predict subsequent nonresponse to continued treatment with the same medication to be associated with poorer outcomes and higher health care costs. Identifying early nonresponders may minimize prolonging exposure to suboptimal or ineffective treatment strategies.
机译:目的:在以精神分裂症为主的急性住院患者的随机对照试验中评估,早期对精神病药无反应似乎可以预测对治疗的后续反应。这项研究评估了早期无反应的预测准确性及其在以精神分裂症为主的慢性门诊病人的自然疗法中的临床,功能和经济影响。方法:这项事后分析使用了为期1年的随机,开放标签研究的奥氮平,利培酮和典型抗精神病药治疗精神分裂症的数据。如果临床需要,患者可以在治疗8周后更换抗精神病药。包括完成治疗8周的患者(n = 664名患者中的443名)。将早期反应(在2周时阳性和阴性综合征量表比基线改善≥20%)的患者与早期无反应者在8周时的症状缓解,功能,对药物影响的感知以及总医疗费用进行比较。结果:2周时的早期反应/无反应预测了8周时的后续反应/无反应,其准确性(72%)和特异性(89%)很高。 8周后,早期无反应者不太可能实现症状缓解(P <.001),功能域改善较少(P <.05),认为药物治疗的效果较差(P = .004),并且产生了总体健康护理费用是早期响应者的两倍(4349美元对2102美元,P = .010)。结论:在精神分裂症患者的常规护理中,早期无反应似乎可以可靠地预测随后对使用相同药物继续治疗的无反应,这与较差的预后和较高的医疗费用有关。识别早期无反应者可以最大程度地减少长时间暴露于次优或无效的治疗策略。

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