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药理学知识在癌症化疗设计与监测中的益处。

Benefits of pharmacological knowledge in the design and monitoring of cancer chemotherapy.

作者信息

Canal P, Gamelin E, Vassal G, Robert J

机构信息

Centre Claudius-Regaud, Toulouse, France.

出版信息

Pathol Oncol Res. 1998;4(3):171-8. doi: 10.1007/BF02905246.

Abstract

Prescribing chemotherapy is a difficult task, because of drug resistance, which prevents all tumors to respond to a given protocol and because of drug toxicity, which is generally unavoidable but which must be limited to acceptable levels. The therapeutic window of anticancer drugs is very narrow and clinicians have to try to optimize the individual doses and schedules of the drugs to be administered. They can rely upon simple anthropometric features, such as body weight or surface area; they can also take into account the physiological status of the patient: age, liver and kidney function, genetic characteristics of drug metabolism, etc. The best way for dose adaptation lies in the establishment of pharmacokinetic/pharmacodynamic relationships, i.e., between the behavior of a drug in the body and its efficacy and toxicity. When it is established that the optimal effect of a drug is related to a given parameter, such as the area under the curve plotting plasma concentration vs. time (AUC), it becomes possible to administer the drug with the dose allowing to obtain the target parameter value. Individual dose adaptation can be achieved thanks to the study of the pharmacokinetics of a test dose preceding that of the therapeutic dose, or by the measure of drug plasma levels, either at steady state during a protracted infusion, or from cycle to cycle during repetitive protocols. Population analysis now allows the adaptation of anticancer drug dosing from a minimum knowledge of individual pharmacokinetic features, together with other characteristics of the patients such as age, gender or physiological functions.

摘要

开具化疗药物是一项艰巨的任务,这是因为存在耐药性,它会阻碍所有肿瘤对给定方案产生反应;还因为存在药物毒性,这通常不可避免,但必须将其限制在可接受的水平。抗癌药物的治疗窗口非常狭窄,临床医生必须努力优化待给药药物的个体化剂量和给药方案。他们可以依据简单的人体测量特征,如体重或体表面积;也可以考虑患者的生理状况:年龄、肝肾功能、药物代谢的遗传特征等。剂量调整的最佳方法在于建立药代动力学/药效学关系,即在药物在体内的行为与其疗效和毒性之间建立关系。当确定一种药物的最佳疗效与某个给定参数相关时,例如绘制血浆浓度与时间关系的曲线下面积(AUC),就可以给予能获得目标参数值的剂量来给药。通过研究治疗剂量之前的试验剂量的药代动力学,或者通过测量药物血浆水平(在长时间输注期间的稳态时,或在重复给药方案期间的不同周期之间),可以实现个体化剂量调整。群体分析现在允许从对个体药代动力学特征的最少了解以及患者的其他特征(如年龄、性别或生理功能)来调整抗癌药物的剂量。

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