Quantitative Pharmacology Approach to Select Optimal Dose and Study the Important Factors in Determining Disposition of Therapeutic Monoclonal Antibody in Pediatric Subjects – Some Considerations

“…Excluding mAbs that have received concurrent initial pediatric indication with adult approval, time lag in the approval of new treatment between adults and children is approximately 5.8 years (range, 1‐12 years). Efforts need to be taken to expedite pediatric drug development and modeling and simulation can play an important role, by improving pediatric trial efficiency, optimizing dose selection, and informing extrapolation‐based drug development from adults to children 2‐6 …”

“…Efforts need to be taken to expedite pediatric drug development and modeling and simulation can play an important role, by improving pediatric trial efficiency, optimizing dose selection, and informing extrapolation-based drug development from adults to children. [2][3][4][5][6] The importance of pharmacokinetic (PK) evaluation in pediatric drug development is well recognized, and a pediatric PK study is generally recommended before pivotal pediatric trials to ensure the "right" dose in these studies. [7][8][9] The PK of mAbs is primarily affected by body weight, and extrapolation from adults to children may conform to allometry.…”

Model‐Aided Adults‐to‐Children Pharmacokinetic Extrapolation and Empirical Body Size‐Based Dosing Exploration for Therapeutic Monoclonal Antibodies—Is Allometry a Reasonable Choice?

“…Excluding mAbs that have received concurrent initial pediatric indication with adult approval, time lag in the approval of new treatment between adults and children is approximately 5.8 years (range, 1‐12 years). Efforts need to be taken to expedite pediatric drug development and modeling and simulation can play an important role, by improving pediatric trial efficiency, optimizing dose selection, and informing extrapolation‐based drug development from adults to children 2‐6 …”

“…Efforts need to be taken to expedite pediatric drug development and modeling and simulation can play an important role, by improving pediatric trial efficiency, optimizing dose selection, and informing extrapolation-based drug development from adults to children. [2][3][4][5][6] The importance of pharmacokinetic (PK) evaluation in pediatric drug development is well recognized, and a pediatric PK study is generally recommended before pivotal pediatric trials to ensure the "right" dose in these studies. [7][8][9] The PK of mAbs is primarily affected by body weight, and extrapolation from adults to children may conform to allometry.…”

Model‐Aided Adults‐to‐Children Pharmacokinetic Extrapolation and Empirical Body Size‐Based Dosing Exploration for Therapeutic Monoclonal Antibodies—Is Allometry a Reasonable Choice?