Abstract
Extrapolation of pharmacokinetic (PK) parameters from in vitro or in vivo animal to human is one of the main tasks in the drug development process. Translational approaches provide evidence for go or no-go decision-making during drug discovery and the development process, and the prediction of human PKs prior to the first-in-human clinical trials. In vitro-in vivo extrapolation and allometric scaling are the choice of method for projection to human situations. Although these methods are useful tools for the estimation of PK parameters, it is a challenge to apply these methods since underlying biochemical, mathematical, physiological, and background knowledge of PKs are required. In addition, it is difficult to select an appropriate methodology depending on the data available. Therefore, this review covers the principles of PK parameters pertaining to the clearance, volume of distribution, elimination half-life, absorption rate constant, and prediction method from the original idea to recently developed models in order to introduce optimal models for the prediction of PK parameters.
Reference131 articles.
1. Pharmaceutical innovation by the seven UK-owned pharmaceutical companies (1964-1985).
2. The pivotal role of drug metabolism and pharmacokinetics in the discovery and development of new medicines;Alavijeh;Curr. Opin. Investig. Drugs,2004
3. Phase II and phase III failures: 2013–2015
4. Can the pharmaceutical industry reduce attrition rates?
5. The impact of early ADME profiling on drug discovery and development strategy;Wang;Drug Discov. World,2004
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