Monoclonal Antibodies and Fc‐Fusion Proteins for Pediatric Use: Dosing, Immunogenicity, and Modeling and Simulation in Data Submitted to the US Food and Drug Administration

The experience with the use of monoclonal antibodies and Fc‐fusion proteins (mAb/Fc) in the pediatric population is limited. The objective of this study is to review those factors impacting the clinical efficacy and product safety of mAb/Fc products in pediatric patients during drug development. We...

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Published inJournal of clinical pharmacology Vol. 59; no. 8; pp. 1130 - 1143
Main Authors Liu, Xiaomei I., Dallmann, André, Wang, Yow‐Ming, Green, Dionna J., Burnham, Janelle M., Chiang, Beatrice, Wu, Perry, Sheng, Mark, Lu, Kelley, Anker, John N., Burckart, Gilbert J.
Format Journal Article
LanguageEnglish
Published England 01.08.2019
Subjects
dosing
drug development
Fc‐fusion proteins
immunogenicity
modeling and simulation
monoclonal antibodies
pediatrics
modeling and simulation
pediatrics
drug development
Fc-fusion proteins
dosing
immunogenicity
monoclonal antibodies
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Abstract The experience with the use of monoclonal antibodies and Fc‐fusion proteins (mAb/Fc) in the pediatric population is limited. The objective of this study is to review those factors impacting the clinical efficacy and product safety of mAb/Fc products in pediatric patients during drug development. We reviewed the list of biologic products in the US Food and Drug Administration's Purple Book as of March 2018 with a focus on mAb/Fc products that are indicated for use in both adults and pediatric patients. Of 68 mAb/Fc products in the Purple Book (excluding biosimilars), 20 products have approved indications in both adults and children. Thirteen products had concurrent approval for both adult and pediatric populations. The sample size of pediatric studies generally ranged from approximately 2% to 70% of the sample size of adult studies with the same indication. In general, pediatric dosing regimens were found to be more based on body weight and weight tiered than the regimens for adults. Modeling and simulation techniques comprised mainly population pharmacokinetic and pharmacodynamic models. A review of the immunogenicity incidence did not reveal any notable difference in the 5 products having data on both pediatric and adult patients. In conclusion, most of the mAb/Fc products have a different weight‐based dosing regimen for pediatric patients versus adults. An understanding of the comparative experience in drug development for mAb/Fc products between adult and pediatric patients coupled with the application of advanced modeling and simulation methods should assist future development of new mAb/Fc products for pediatric patients.
AbstractList The experience with the use of monoclonal antibodies and Fc‐fusion proteins (mAb/Fc) in the pediatric population is limited. The objective of this study is to review those factors impacting the clinical efficacy and product safety of mAb/Fc products in pediatric patients during drug development. We reviewed the list of biologic products in the US Food and Drug Administration's Purple Book as of March 2018 with a focus on mAb/Fc products that are indicated for use in both adults and pediatric patients. Of 68 mAb/Fc products in the Purple Book (excluding biosimilars), 20 products have approved indications in both adults and children. Thirteen products had concurrent approval for both adult and pediatric populations. The sample size of pediatric studies generally ranged from approximately 2% to 70% of the sample size of adult studies with the same indication. In general, pediatric dosing regimens were found to be more based on body weight and weight tiered than the regimens for adults. Modeling and simulation techniques comprised mainly population pharmacokinetic and pharmacodynamic models. A review of the immunogenicity incidence did not reveal any notable difference in the 5 products having data on both pediatric and adult patients. In conclusion, most of the mAb/Fc products have a different weight‐based dosing regimen for pediatric patients versus adults. An understanding of the comparative experience in drug development for mAb/Fc products between adult and pediatric patients coupled with the application of advanced modeling and simulation methods should assist future development of new mAb/Fc products for pediatric patients.
Author Sheng, Mark
Anker, John N.
Dallmann, André
Wang, Yow‐Ming
Lu, Kelley
Burckart, Gilbert J.
Burnham, Janelle M.
Green, Dionna J.
Chiang, Beatrice
Wu, Perry
Liu, Xiaomei I.
Author_xml – sequence: 1
  givenname: Xiaomei I.
  surname: Liu
  fullname: Liu, Xiaomei I.
  organization: Children's National Medical Center
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  givenname: André
  surname: Dallmann
  fullname: Dallmann, André
  organization: University Children's Hospital Basel (UKBB)
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  givenname: Yow‐Ming
  surname: Wang
  fullname: Wang, Yow‐Ming
  organization: US Food and Drug Administration
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  givenname: Dionna J.
  surname: Green
  fullname: Green, Dionna J.
  organization: US Food and Drug Administration
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  givenname: Janelle M.
  surname: Burnham
  fullname: Burnham, Janelle M.
  organization: US Food and Drug Administration
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  givenname: Beatrice
  surname: Chiang
  fullname: Chiang, Beatrice
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  fullname: Wu, Perry
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  givenname: Mark
  surname: Sheng
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  organization: University of Southern California
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  organization: University Children's Hospital Basel (UKBB)
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  givenname: Gilbert J.
  surname: Burckart
  fullname: Burckart, Gilbert J.
  email: Gilbert.Burckart@fda.hhs.gov
  organization: US Food and Drug Administration
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Issue 8
Keywords modeling and simulation
pediatrics
drug development
Fc-fusion proteins
dosing
immunogenicity
monoclonal antibodies
Language English
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2019 The Authors. The Journal of Clinical Pharmacology published by Wiley Periodicals, Inc. on behalf of American College of Clinical Pharmacology.
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Snippet The experience with the use of monoclonal antibodies and Fc‐fusion proteins (mAb/Fc) in the pediatric population is limited. The objective of this study is to...
The experience with the use of monoclonal antibodies and Fc-fusion proteins (mAb/Fc) in the pediatric population is limited. The objective of this study is to...
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StartPage 1130
SubjectTerms dosing
drug development
Fc‐fusion proteins
immunogenicity
modeling and simulation
monoclonal antibodies
pediatrics
Title Monoclonal Antibodies and Fc‐Fusion Proteins for Pediatric Use: Dosing, Immunogenicity, and Modeling and Simulation in Data Submitted to the US Food and Drug Administration
URI https://onlinelibrary.wiley.com/doi/abs/10.1002%2Fjcph.1406
https://www.ncbi.nlm.nih.gov/pubmed/30865317
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