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首页> 外文期刊>Early intervention in psychiatry >NEURAPRO‐E study protocol: a multicentre randomized controlled trial of omega‐3 fatty acids and cognitive‐behavioural case management for patients at ultra high risk of schizophrenia and other psychotic disorders
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NEURAPRO‐E study protocol: a multicentre randomized controlled trial of omega‐3 fatty acids and cognitive‐behavioural case management for patients at ultra high risk of schizophrenia and other psychotic disorders

机译:Neuropro-E研究方案:欧米茄3脂肪酸的多期随机对照试验,对精神分裂症和其他精神病患者的超高危患者的患者的认知行为案例管理

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Abstract Aim Recent research has indicated that preventative intervention is likely to benefit patients ‘at‐risk’ for psychosis, both in terms of symptom reduction and delay or prevention of onset of threshold psychotic disorder. The strong preliminary results for the effectiveness of omega‐3 polyunsaturated fatty acids ( PUFA s), coupled with the falling transition rate in ultra high‐risk ( UHR ) samples, mean that further study of such benign, potentially neuroprotective interventions is clinically and ethically required. Employing a multicentre approach, enabling a large sample size, this study will provide important information with regard to the use of omega‐3 PUFAs in the UHR group. Methods This trial is a 6‐month, double‐blind, randomized placebo‐controlled trial of 1.4 g day ?1 omega‐3 PUFAs in UHR patients aged between 13 and 40 years. The primary hypothesis is that UHR patients receiving omega‐3 PUFAs plus cognitive‐behavioural case management ( CBCM ) will be less likely to transition to psychosis over a 6‐month period compared to treatment with placebo plus CBCM . Secondary outcomes will examine symptomatic and functional changes, as well as examine if candidate risk factors predict response to omega‐3 PUFA treatment in the UHR group. Conclusion This is the protocol of the NeuraproE study. Utilizing a large sample, results from this study will be important in informing indicated prevention strategies for schizophrenia and other psychotic disorders, which may be the strongest avenue for reducing the burden, stigmatization, disability and economic consequences of these disorders.
机译:摘要目的最近的研究表明,在症状减少和延迟或预防门槛精神病障碍的症状方面,预防性干预可能会使患者为精神病患者进行精神病。 ω-3多不饱和脂肪酸(PUFA S)有效性的强烈初步结果与超高风险(UHR)样品中的下降过渡率相结合,意味着进一步研究这种良性,可能是神经保护干预措施在临床上和道德上必需的。采用多中心的方法,实现大型样本量,本研究将提供关于在UHR组中使用Omega-3 Pufas的重要信息。方法本试验是6个月,双盲,随机安慰剂对照试验1.4克(13至40岁)的UHR患者中的1兆-3普菲斯。主要假设是接受OMEGA-3 PUFA加上认知行为案例管理(CBCM)的UHR患者在6个月内与安慰剂加上CBCM的治疗相比,对精神病的可能性不太可能过渡到精神病。二次结果将研究症状和功能变化,以及审查候选风险因素是否预测UHR组对ω-3 PUFA治疗的反应。结论这是Neuroproe研究的协议。利用大型样品,本研究的结果对于通知精神分裂症和其他精神病疾病的预防策略,这可能是最强的途径,这可能是降低这些障碍的负担,侮辱,残疾和经济后果的最强的途径。

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