阿立哌唑和利培酮治疗首发非情感性精神病的疗效比较:一项前瞻性、随机、3期、研究者启动的研究(PAFIP-3)的基本原理和设计

Mayoral-van Son J. , Marcos Gómez-Revuelta , Rosa Ayesa-Arriola , Javier Vázquez-Bourgón , Víctor Ortiz-García de la Foz , Miguel Ruiz-Veguilla , Nathalia Garrido , Diana Tordesillas-Gutiérrez , Esther Setién-Suero , Benedicto Crespo-Facorro
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引用次数: 0

摘要

背景:选择最有效的治疗方法是一项关键的挑战,有可能改变初次精神病发作患者的长期预后。比较抗精神病药物对首发非情感性精神病(FEP)个体疗效的正面临床试验很少。方法报告一项三期临床试验(PAFIP-3, NCT02305823)的基本原理和设计,比较阿立哌唑和利培酮的有效性,并评估早期使用氯氮平对原发性治疗耐药患者的益处。该设计包括5个工作包(药物算法、认知功能、心理教育/职业功能、成像和生物标记),解决首发精神病患者及其护理的关键问题和需求。主要结局指标是通过全因治疗停药率评估治疗效果。结果266人被纳入随机化研究I期(利培酮vs阿立哌唑)。在3个月时,保留率为94%(249/266),48例(19.3%)患者通过了II期(奥氮平治疗),7例(2.8%)患者进入氯氮平期(III期)。讨论PAFIP 3临床试验可能为临床指南提供相关信息,以最佳地治疗首次发作的非情感性精神病患者,以及早期使用氯氮平治疗耐药患者的益处和风险。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Comparison of aripiprazole and risperidone effectiveness in first episode non-affective psychosis: Rationale and design of a prospective, randomized, 3-phase, investigator-initiated study (PAFIP-3)

Background

Selecting the most effective treatment represents a critical challenge with the potential of modifying the long-term prognosis of individuals suffering a first break of psychosis. Head-to-head clinical trials comparing effectiveness among antipsychotic drugs in individuals with a first-episode of non-affective psychosis (FEP) are scarce.

Methods

The rationale and design of a 3 phases clinical trial (PAFIP-3, NCT02305823) comparing the effectiveness of aripiprazole and risperidone, and to additionally assess the benefits of an early use of clozapine in primary treatment-resistant patients is reported. The design encompasses of 5 work packages (medication algorithm, cognitive functioning, psychoeducation/vocational functioning, imaging and biological markers) addressing critical issues and needs of first episode psychosis individuals and their cares. The primary outcome measure was treatment effectiveness assessed by all-cause treatment discontinuation rate.

Results

266 individuals have been included in the randomization study phase I (risperidone vs. aripiprazole). At 3 months, the retention rate was of 94% (249/266), 48(19.3%) patients have gone through phase II (olanzapine treatment), and 7(2.8%) entered the clozapine phase (phase III).

Discussion

The PAFIP 3 clinical trial may provide relevant information about clinical guidelines to optimally treat patients with a first episode of non-affective psychosis and the benefits and risks of an early use of clozapine in treatment resistant patients.

Clinicaltrials.gov: NCT02305823.

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