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德克萨斯药物算法项目治疗精神分裂症的抗精神病药物算法:2006年更新版。

The Texas Medication Algorithm Project antipsychotic algorithm for schizophrenia: 2006 update.

作者信息

Moore Troy A, Buchanan Robert W, Buckley Peter F, Chiles John A, Conley Robert R, Crismon M Lynn, Essock Susan M, Finnerty Molly, Marder Stephen R, Miller Del D, McEvoy Joseph P, Robinson Delbert G, Schooler Nina R, Shon Steven P, Stroup T Scott, Miller Alexander L

机构信息

Department of Psychiatry, The University of Texas Health Science Center at San Antonio, USA.

出版信息

J Clin Psychiatry. 2007 Nov;68(11):1751-62. doi: 10.4088/jcp.v68n1115.

Abstract

BACKGROUND

A panel of academic psychiatrists and pharmacists, clinicians from the Texas public mental health system, advocates, and consumers met in June 2006 in Dallas, Tex., to review recent evidence in the pharmacologic treatment of schizophrenia. The goal of the consensus conference was to update and revise the Texas Medication Algorithm Project (TMAP) algorithm for schizophrenia used in the Texas Implementation of Medication Algorithms, a statewide quality assurance program for treatment of major psychiatric illness.

METHOD

Four questions were identified via premeeting teleconferences. (1) Should antipsychotic treatment of first-episode schizophrenia be different from that of multiepisode schizophrenia? (2) In which algorithm stages should first-generation antipsychotics (FGAs) be an option? (3) How many antipsychotic trials should precede a clozapine trial? (4) What is the status of augmentation strategies for clozapine? Subgroups reviewed the evidence in each area and presented their findings at the conference.

RESULTS

The algorithm was updated to incorporate the following recommendations. (1) Persons with first-episode schizophrenia typically require lower antipsychotic doses and are more sensitive to side effects such as weight gain and extrapyramidal symptoms (group consensus). Second-generation antipsychotics (SGAs) are preferred for treatment of first-episode schizophrenia (majority opinion). (2) FGAs should be included in algorithm stages after first episode that include SGAs other than clozapine as options (group consensus). (3) The recommended number of trials of other antipsychotics that should precede a clozapine trial is 2, but earlier use of clozapine should be considered in the presence of persistent problems such as suicidality, comorbid violence, and substance abuse (group consensus). (4) Augmentation is reasonable for persons with inadequate response to clozapine, but published results on augmenting agents have not identified replicable positive results (group consensus).

CONCLUSIONS

These recommendations are meant to provide a framework for clinical decision making, not to replace clinical judgment. As with any algorithm, treatment practices will evolve beyond the recommendations of this consensus conference as new evidence and additional medications become available.

摘要

背景

2006年6月,一群学术精神病学家、药剂师、得克萨斯州公共精神卫生系统的临床医生、倡导者和消费者在得克萨斯州达拉斯市会面,审查精神分裂症药物治疗的最新证据。此次共识会议的目标是更新和修订用于《得克萨斯州药物治疗算法实施项目》(TMAP)的精神分裂症算法,该项目是一项针对重度精神疾病治疗的全州质量保证计划。

方法

通过会前电话会议确定了四个问题。(1)首发精神分裂症的抗精神病药物治疗是否应与多发型精神分裂症不同?(2)在算法的哪些阶段,第一代抗精神病药物(FGAs)应作为一种选择?(3)在进行氯氮平试验之前应进行多少次抗精神病药物试验?(4)氯氮平的增效策略的现状如何?各小组审查了每个领域的证据,并在会议上展示了他们的研究结果。

结果

算法得到更新,纳入了以下建议。(1)首发精神分裂症患者通常需要较低剂量的抗精神病药物,并且对体重增加和锥体外系症状等副作用更敏感(小组共识)。第二代抗精神病药物(SGAs)是首发精神分裂症治疗的首选(多数意见)。(2)FGAs应纳入首发后算法阶段,该阶段包括除氯氮平以外的SGAs作为选择(小组共识)。(3)在进行氯氮平试验之前,推荐的其他抗精神病药物试验次数为2次,但在存在自杀倾向、合并暴力和药物滥用等持续问题的情况下,应考虑更早使用氯氮平(小组共识)。(4)对于氯氮平反应不足的患者,增效是合理的,但关于增效剂的已发表结果尚未确定可重复的阳性结果(小组共识)。

结论

这些建议旨在为临床决策提供一个框架,而不是取代临床判断。与任何算法一样,随着新证据和更多药物的出现,治疗实践将超越本次共识会议的建议而不断发展。

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