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药物相互作用导致化疗药物药代动力学特征的改变。

Alterations of chemotherapeutic pharmacokinetic profiles by drug-drug interactions.

机构信息

Albert Einstein College of Medicine, Albert Einstein Cancer Center, Bronx, NY 10461, USA.

出版信息

Expert Opin Drug Metab Toxicol. 2009 Feb;5(2):109-30. doi: 10.1517/17425250902753212.

Abstract

BACKGROUND

Drug interactions in oncology are common place and largely ignored as we tolerate high thresholds of 'toxic' drug responses in these patients. However, in the era of 'targeted' or seemingly 'less toxic' therapy, these interactions are more commonly flagged and contribute significantly towards poor 'quality of life' and medical fatalities.

OBJECTIVE

This review and opinion article focuses on alteration of chemotherapeutic pharmacokinetic profiles by drug interactions in the setting of polypharmacy. The assumption is that the drugs, with changes in their pharmacokinetics, will contribute towards changes in their pharmacodynamics.

METHODS

The examples cited for such drug-drug interactions are culled from published literature with an emphasis on those interactions that have been well characterized at the molecular level.

RESULTS

Although very few drug interaction studies have been performed on approved oncology based drugs, it is clear that drugs whose pharmacokinetics profiles are closely related to their pharmacodynamics will indeed result in clinically important drug interactions. Some newer mechanisms are described that involve interactions at the level of gene transcription, whereby, drug metabolism is significantly altered. However, for any given drug interaction, there does not seem to be a comprehensive model describing interactions.

CONCLUSIONS

Mechanisms based drug interactions are plentiful in oncology; however, there is an absolute lack of a comprehensive model that would predict drug-drug interactions.

摘要

背景

肿瘤学中的药物相互作用很常见,但由于我们对这些患者的“毒性”药物反应容忍度较高,因此很大程度上被忽视了。然而,在“靶向”或看似“毒性较低”的治疗时代,这些相互作用更为常见,并显著导致较差的“生活质量”和医疗死亡。

目的

本文回顾和讨论了药物相互作用在多药治疗情况下对化疗药药代动力学的影响。假设是,药物的药代动力学发生变化,将导致其药效学发生变化。

方法

所引用的此类药物相互作用的例子均来自已发表的文献,重点介绍了那些在分子水平上得到充分描述的相互作用。

结果

尽管很少有关于已批准的肿瘤学药物的药物相互作用研究,但很明显,那些药代动力学与药效学密切相关的药物确实会导致临床上重要的药物相互作用。描述了一些较新的机制,涉及基因转录水平的相互作用,从而显著改变药物代谢。然而,对于任何给定的药物相互作用,似乎都没有一个全面的模型来描述相互作用。

结论

肿瘤学中存在大量基于机制的药物相互作用,但绝对缺乏能够预测药物相互作用的全面模型。

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