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Optimizing drug development of anti-cancer drugs in children using modelling and simulation
Authors:Johan GC van Hasselt  Natasha KA van Eijkelenburg  Jos H Beijnen  Jan HM Schellens  Alwin DR Huitema
Affiliation:1.Department of Clinical Pharmacology, Netherlands Cancer Institute, Amsterdam;2.Department of Pharmacy & Pharmacology, Slotervaart Hospital/Netherlands Cancer Institute, Amsterdam;3.Department of Pediatric Oncology, Emma Children''s Hospital, Amsterdam;4.Science Faculty, Department of Pharmaceutical Sciences, Division of Pharmacoepidemiology & Clinical Pharmacology, Utrecht University, Utrecht, The Netherlands
Abstract:Modelling and simulation (M&S)-based approaches have been proposed to support paediatric drug development in order to design and analyze clinical studies efficiently. Development of anti-cancer drugs in the paediatric population is particularly challenging due to ethical and practical constraints. We aimed to review the application of M&S in the development of anti-cancer drugs in the paediatric population, and to identify where M&S-based approaches could provide additional support in paediatric drug development of anti-cancer drugs. A structured literature search on PubMed was performed. The majority of identified M&S-based studies aimed to use population PK modelling approaches to identify determinants of inter-individual variability, in order to optimize dosing regimens and to develop therapeutic drug monitoring strategies. Prospective applications of M&S approaches for PK-bridging studies have scarcely been reported for paediatric oncology. Based on recent developments of M&S in drug development there are several opportunities where M&S could support more informative bridging between children and adults, and increase efficiency of the design and analysis of paediatric clinical trials, which should ultimately lead to further optimization of drug treatment strategies in this population.
Keywords:anti-cancer drugs   chemotherapy   modelling   paediatric drug development   paediatric oncology   pharmacokinetics
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