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临床肾脏病药代动力学:基础原理。

Clinical Pharmacokinetics in Kidney Disease: Fundamental Principles.

机构信息

Nephrology and Transplantation Unit, John Hunter Hospital, Newcastle, New South Wales, Australia.

Department of Renal Medicine, The Canberra Hospital, Woden, Australian Capital Territory, Australia; and.

出版信息

Clin J Am Soc Nephrol. 2018 Jul 6;13(7):1085-1095. doi: 10.2215/CJN.00340118. Epub 2018 Jun 22.

Abstract

Kidney disease is an increasingly common comorbidity that alters the pharmacokinetics of many drugs. Prescribing to patients with kidney disease requires knowledge about the drug, the extent of the patient's altered physiology, and pharmacokinetic principles that influence the design of dosing regimens. There are multiple physiologic effects of impaired kidney function, and the extent to which they occur in an individual at any given time can be difficult to define. Although some guidelines are available for dosing in kidney disease, they may be on the basis of limited data or not widely applicable, and therefore, an understanding of pharmacokinetic principles and how to apply them is important to the practicing clinician. Whether kidney disease is acute or chronic, drug clearance decreases, and the volume of distribution may remain the same or increase. Although in CKD, these changes progress relatively slowly, they are dynamic in AKI, and recovery is possible depending on the etiology and treatments. This, and the use of kidney replacement therapies further complicate attempts to quantify drug clearance at the time of prescribing and dosing in AKI. The required change in the dosing regimen can be estimated or even quantitated in certain instances through the application of pharmacokinetic principles to guide rational drug dosing. This offers an opportunity to provide personalized medical care and minimizes adverse drug events from either under- or overdosing. We discuss the principles of pharmacokinetics that are fundamental for the design of an appropriate dosing regimen in this review.

摘要

肾脏疾病是一种越来越常见的合并症,会改变许多药物的药代动力学。为患有肾脏疾病的患者开处方需要了解药物、患者生理改变的程度以及影响剂量方案设计的药代动力学原则。肾功能受损有多种生理影响,在任何特定时间,它们在个体中的发生程度都难以确定。尽管有一些关于肾脏疾病剂量的指南,但它们可能基于有限的数据或不具有广泛适用性,因此,了解药代动力学原则及其应用对临床医生很重要。无论肾脏疾病是急性的还是慢性的,药物清除率都会降低,而分布容积可能保持不变或增加。虽然在 CKD 中,这些变化相对缓慢,但在 AKI 中是动态的,并且根据病因和治疗方法,恢复是可能的。这一点以及肾脏替代疗法的使用,进一步使人们难以在 AKI 时定量确定药物清除率并进行剂量调整。通过应用药代动力学原则来指导合理的药物剂量,可以在某些情况下估计甚至定量计算出剂量方案所需的改变。这为提供个性化医疗护理提供了机会,并最大限度地减少了因剂量不足或过量而导致的药物不良事件。我们在本综述中讨论了药代动力学的基本原理,这些原理是设计适当剂量方案的基础。

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