Bevacizumab dosing strategy in paediatric cancer patients based on population pharmacokinetic analysis with external validation

Kelong Han; Thomas Peyret; Angelica Quartino; Nathalie H Gosselin; Sridharan Gururangan; Michela Casanova; Johannes H M Merks; Maura Massimino; Jacques Grill; Najat C Daw; Fariba Navid; Jin Jin; David E Allison

doi:10.1111/bcp.12778

Bevacizumab dosing strategy in paediatric cancer patients based on population pharmacokinetic analysis with external validation

Br J Clin Pharmacol. 2016 Jan;81(1):148-60. doi: 10.1111/bcp.12778. Epub 2015 Dec 10.

Authors

Affiliations

¹ Clinical Pharmacology, Genentech Inc., South San Francisco, CA, USA.
² Pharsight Consulting Services, Montreal, QC, Canada.
³ Preston Robert Tisch Brain Tumor Center, Duke University Medical Center, Durham, NC.
⁴ Pediatric Oncology Unit, Fondazione IRCCS Istituto Nazionale dei Tumori, Milano, Italy.
⁵ Department of Pediatric Oncology, Emma Children's Hospital-Academic Medical Center (EKZ-AMC), Amsterdam, The Netherlands.
⁶ Gustave Roussy, Faculté de Médecine, University Paris-SUD, Villejuif, France.
⁷ Division of Pediatrics, MD Anderson Cancer Center, Houston, TX.
⁸ Department of Oncology, St Jude Children's Research Hospital, Memphis, TN, USA.

Abstract

Aim: The aim of the present study was to evaluate the pharmacokinetics of bevacizumab and various dosing strategies for this agent in paediatric patients.

Methods: Data were collected from 232 paediatric patients (1971 concentrations) in five studies, with a wide range of age (0.5-21 years), body weight (BWT; 5.9-125 kg), and regimens (5-15 mg kg(-1) biweekly or triweekly). Data from 152 patients (1427 concentrations) and 80 patients (544 concentrations) were used for model building and external validation, respectively. Steady-state exposure was simulated under BWT-based, body surface area (BSA)-based, ideal body weight (IBW)-based, and tier-based doses. NONMEM and R were used for analyses.

Results: Typical estimates of clearance, central volume of distribution (V1), and median half-life were 9.04 ml h(-1) , 2851 ml, and 19.6 days, respectively. Clearance decreased with increasing albumin. Clearance and V1 increased with BWT and were higher in male patients. Clearance and V1 were lower in children with primary central nervous system (CNS) tumours than in children with sarcomas, resulting in 49% higher trough (C min) and 29% higher peak (Cmax) concentrations. BWT-adjusted clearance and V1 remained unchanged across ages. Paediatric C min was similar to adult C min under all dosing strategies. Paediatric Cmax exceeded adult Cmax under tier-based doses.

Conclusions: BWT-adjusted pharmacokinetic parameter estimates in paediatric patients were similar to those in adults, and similar across ages. Bevacizumab exposure was higher in children with primary CNS tumours than in children with sarcomas. BSA-based, IBW-based, and tier-based doses offered no substantial advantage over the BWT-based dose currently used in adults for bevacizumab. Given the similarity in pharmacokinetics among many monoclonal antibodies, this may help to develop practical paediatric dosing guidelines for other therapeutic antibodies.

Keywords: bevacizumab; body surface area; central nervous system tumour; dosing strategy; external validation; paediatric.

Publication types

Validation Study

MeSH terms

Adolescent
Angiogenesis Inhibitors / administration & dosage*
Bevacizumab / administration & dosage*
Bevacizumab / pharmacokinetics
Body Weight
Child
Child, Preschool
Humans
Infant
Models, Biological
Neoplasms / drug therapy*
Practice Guidelines as Topic
Young Adult

Substances

Angiogenesis Inhibitors
Bevacizumab

Abstract

Publication types

MeSH terms

Substances

Grants and funding