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血浆氯氮平水平的临床应用。

The clinical use of plasma clozapine levels.

作者信息

Bell R, McLaren A, Galanos J, Copolov D

机构信息

Mental Health Research Institute, Parkville, Victoria, Australia.

出版信息

Aust N Z J Psychiatry. 1998 Aug;32(4):567-74. doi: 10.3109/00048679809068332.

Abstract

OBJECTIVE

This review examines the evidence supporting the proposition that a threshold clozapine plasma level can predict clinical response. In addition, it provides a brief overview of the pharmacokinetics, side effects, drug interactions and assay methodology of clozapine.

METHOD

A comprehensive search of relevant literature was made with respect to the above criteria. The findings were collated and analysed to produce an overview of the usefulness of using clozapine levels in clinical practice.

RESULTS

Most researchers find that, although the correlation between dose of clozapine and clinical effect is not high, a threshold plasma level of 350-420 ng mL-1 of clozapine is associated with an increased probability of a good clinical response to the drug. Results vary, however, with the study design.

CONCLUSIONS

The data reviewed present a case for increasing the dose of clozapine in non-responsive patients to achieve a plasma level of at least 350-420 ng mL-1. Non-response at these levels, however, should not preclude a further upward titration of dose. This should occur unless (i) clinical response is obtained at a lower dose, (ii) intolerable side effects occur, or (iii) a daily dose of 900 mg is reached.

摘要

目的

本综述考察支持氯氮平血浆阈值水平可预测临床反应这一观点的证据。此外,还简要概述氯氮平的药代动力学、副作用、药物相互作用及检测方法。

方法

按照上述标准对相关文献进行全面检索。对研究结果进行整理和分析,以概述在临床实践中使用氯氮平血药浓度的实用性。

结果

大多数研究人员发现,尽管氯氮平剂量与临床疗效之间的相关性不高,但氯氮平血浆阈值水平为350 - 420 ng/mL时,药物产生良好临床反应的可能性增加。然而,结果因研究设计而异。

结论

所综述的数据表明,对于无反应的患者,应增加氯氮平剂量以达到至少350 - 420 ng/mL的血浆水平。然而,在这些水平上无反应不应排除进一步向上滴定剂量。除非出现以下情况,否则应进行剂量滴定:(i) 在较低剂量时获得临床反应,(ii) 出现无法耐受的副作用,或(iii) 达到每日900 mg的剂量。

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