The value of drug and metabolite concentration in blood as a biomarker of psychopharmacological therapy.

Gudrun Hefner, A Kathrin Laib, Hilmar Sigurdsson, Matthias Hohner, Christoph Hiemke
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引用次数: 24

Abstract

Desirable and undesirable effects of a drug are related to its concentration at various sites of actions. For many psychotropic drugs, it has been shown that drug concentration in brain correlates with concentration in blood. The latter is also an available estimate of clearance and bioavailability. Its monitoring enables identification of multiple factors that have an impact on clinical outcomes, especially uncertain compliance and pharmacokinetic peculiarities. For this review we analysed for antidepressants if drug concentration in blood can be used as biomarker for psychopharmacological treatment. Systematic review of the literature revealed for new and old antidepressant drugs that drug and metabolite concentrations in blood are measures of the pharmacokinetic phenotype and related differentially to occupancy of primary target structures, therapeutic effects and unwanted anticholinergic, cardiac and other side effects. Drug concentration in blood can therefore be used as biomarker in clinical practice to guide psychopharmacological treatment with established antidepressant drugs. Monitoring of drug concentration is suitable to improve efficacy and safety of the pharmacotherapy, especially in elderly patients who require complex pharmacological therapies.

血液中药物和代谢物浓度作为精神药物治疗的生物标志物的价值。
一种药物的理想和不理想的效果与它在不同作用部位的浓度有关。对于许多精神药物,已经证明药物在脑中的浓度与血液中的浓度相关。后者也是清除率和生物利用度的可用估计。它的监测可以识别影响临床结果的多种因素,特别是不确定的依从性和药代动力学特性。在这篇综述中,我们分析了抗抑郁药物的血液浓度是否可以作为精神药理学治疗的生物标志物。系统回顾文献发现,对于新旧抗抑郁药物,血液中药物和代谢物浓度是药代动力学表型的衡量指标,与主要靶点结构的占据、治疗效果和不必要的抗胆碱能、心脏和其他副作用存在差异。因此,血液中的药物浓度可以作为临床实践中的生物标志物,指导已建立的抗抑郁药物的精神药理学治疗。药物浓度监测适用于提高药物治疗的疗效和安全性,尤其适用于需要复杂药物治疗的老年患者。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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