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长效抗精神病药物。风险效益评估。

Long-term depot antipsychotics. A risk-benefit assessment.

作者信息

Barnes T R, Curson D A

机构信息

Department of Psychiatry, Charing Cross and Westminster Medical School, London, England.

出版信息

Drug Saf. 1994 Jun;10(6):464-79. doi: 10.2165/00002018-199410060-00005.

Abstract

The main advantage of depot antipsychotic medication is that it overcomes the problem of covert noncompliance. Patients receiving depot treatment who refuse their injection or fail to receive it for any other reason can be immediately identified and appropriate action taken. In the context of a carefully monitored management programme, depot treatment can have a major impact on compliance and, consequently, the risk of relapse and hospitalisation can be reduced. Another major advantage is that the considerable individual variation in bioavailability and metabolism with oral antipsychotic drugs is markedly reduced with depot treatment. A better correlation between the dose administered and the concentration of medication found in blood or plasma is achieved with depot treatment, and thus, the clinician has greater control over the amount of drug being delivered to the site of activity. A further benefit of depot treatment is the achievement of stable plasma concentrations over long periods, allowing injections to be given every few weeks. However, this also represents a potential disadvantage in that there is a lack of flexibility of administration. Should adverse effects develop, the drug cannot be rapidly withdrawn. Furthermore, adjustment to the optimal dose becomes a long term strategy. The controlled studies of low dose maintenance therapy with depot treatment suggest that it can take months or years for the consequences of dose reduction, in terms of increased risk of relapse, to become manifest. When weighing up the risks and benefits of long term antipsychotic treatment for the individual patient with schizophrenia, the clinician must take into account the nature, severity and frequency of past relapses, and the degree of distress and disability related to any adverse effects. However, the clinical decision to prescribe either a depot or an oral antipsychotic for maintenance treatment will probably rest largely on an assessment of the risk of poor compliance in the particular patient. There is no convincing evidence that the range, nature or severity of adverse effects reported with depot treatment is significantly different from that seen with oral treatment, and depot treatment has been shown to be as good or better than oral medication in preventing or postponing relapse. Furthermore, when adjusting the dose or frequency of depot injection, to improve control of psychotic symptoms or reduce adverse effects, the clinician can be confident that the dose prescribed is the dose being received by the patient.

摘要

长效抗精神病药物的主要优点是它克服了隐性不依从的问题。接受长效治疗的患者若拒绝注射或因任何其他原因未能接受注射,能够立即被识别出来,并采取适当措施。在精心监测的管理方案背景下,长效治疗对依从性有重大影响,因此,可以降低复发和住院的风险。另一个主要优点是,与口服抗精神病药物相比,长效治疗可显著减少生物利用度和代谢方面相当大的个体差异。长效治疗能使给药剂量与血液或血浆中药物浓度之间有更好的相关性,因此,临床医生对输送到作用部位的药量有更大的控制权。长效治疗的另一个好处是能在很长一段时间内实现稳定的血浆浓度,允许每隔几周注射一次。然而,这也代表了一个潜在的缺点,即给药缺乏灵活性。如果出现不良反应,药物不能迅速停用。此外,调整到最佳剂量成为一项长期策略。关于长效治疗低剂量维持疗法的对照研究表明,就复发风险增加而言,剂量减少的后果可能需要数月或数年才会显现出来。在权衡对个体精神分裂症患者进行长期抗精神病治疗的风险和益处时,临床医生必须考虑过去复发的性质、严重程度和频率,以及与任何不良反应相关的痛苦和残疾程度。然而,决定开长效或口服抗精神病药物进行维持治疗的临床决策可能很大程度上取决于对特定患者依从性差风险的评估。没有令人信服的证据表明,长效治疗报告的不良反应范围、性质或严重程度与口服治疗有显著差异,并且长效治疗在预防或推迟复发方面已被证明与口服药物一样好或更好。此外,在调整长效注射的剂量或频率以改善对精神病症状的控制或减少不良反应时,临床医生可以确信所开的剂量就是患者所接受的剂量。

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