Waiving in vivo studies for monoclonal antibody biosimilar development: National and global challenges

Biosimilars are biological medicinal products that contain a version of the active substance of an already authorised original biological medicinal product (the innovator or reference product). The first approved biosimilar medicines were small proteins, and more recently biosimilar versions of inno...

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Autores principales: Chapman, Kathryn, Adjei, Akosua, Baldrick, Paul, da Silva, Antonio, De Smet, Karen, DiCicco, Richard, Hong, Seung Suh, Jones, David, Leach, Michael W., McBlane, James, Ragan, Ian, Reddy, Praveen, Stewart, Donald I. H., Suitters, Amanda, Sims, Jennifer
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2016
Materias:
Perspective
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4966840/
https://www.ncbi.nlm.nih.gov/pubmed/26854177
http://dx.doi.org/10.1080/19420862.2016.1145331
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author Chapman, Kathryn
Adjei, Akosua
Baldrick, Paul
da Silva, Antonio
De Smet, Karen
DiCicco, Richard
Hong, Seung Suh
Jones, David
Leach, Michael W.
McBlane, James
Ragan, Ian
Reddy, Praveen
Stewart, Donald I. H.
Suitters, Amanda
Sims, Jennifer
author_facet Chapman, Kathryn
Adjei, Akosua
Baldrick, Paul
da Silva, Antonio
De Smet, Karen
DiCicco, Richard
Hong, Seung Suh
Jones, David
Leach, Michael W.
McBlane, James
Ragan, Ian
Reddy, Praveen
Stewart, Donald I. H.
Suitters, Amanda
Sims, Jennifer
author_sort Chapman, Kathryn
collection PubMed
description Biosimilars are biological medicinal products that contain a version of the active substance of an already authorised original biological medicinal product (the innovator or reference product). The first approved biosimilar medicines were small proteins, and more recently biosimilar versions of innovator monoclonal antibody (mAb) drugs have entered development as patents on these more complex proteins expire. In September 2013, the first biosimilar mAb, infliximab, was authorised in Europe. In March 2015, the first biosimilar (Zarxio™, filgrastim-sndz, Sandoz) was approved by the US Food and Drug Administration; however, to date no mAb biosimilars have been approved in the US. There are currently major differences between how biosimilars are regulated in different parts of the world, leading to substantial variability in the amount of in vivo nonclinical toxicity testing required to support clinical development and marketing of biosimilars. There are approximately 30 national and international guidelines on biosimilar development and this number is growing. The European Union's guidance describes an approach that enables biosimilars to enter clinical trials based on robust in vitro data alone; in contrast, the World Health Organization's guidance is interpreted globally to mean in vivo toxicity studies are mandatory. We reviewed our own experience working in the global regulatory environment, surveyed current practice, determined drivers for nonclinical in vivo studies with biosimilar mAbs and shared data on practice and study design for 25 marketed and as yet unmarketed biosimilar mAbs that have been in development in the past 5y. These data showed a variety of nonclinical in vivo approaches, and also demonstrated the practical challenges faced in obtaining regulatory approval for clinical trials based on in vitro data alone. The majority of reasons for carrying out nonclinical in vivo studies were not based on scientific rationale, and therefore the authors have made recommendations for a data-driven approach to the toxicological assessment of mAb biosimilars that minimises unnecessary use of animals and can be used across all regions of the world.
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spelling pubmed-49668402016-08-23 Waiving in vivo studies for monoclonal antibody biosimilar development: National and global challenges Chapman, Kathryn Adjei, Akosua Baldrick, Paul da Silva, Antonio De Smet, Karen DiCicco, Richard Hong, Seung Suh Jones, David Leach, Michael W. McBlane, James Ragan, Ian Reddy, Praveen Stewart, Donald I. H. Suitters, Amanda Sims, Jennifer MAbs Perspective Biosimilars are biological medicinal products that contain a version of the active substance of an already authorised original biological medicinal product (the innovator or reference product). The first approved biosimilar medicines were small proteins, and more recently biosimilar versions of innovator monoclonal antibody (mAb) drugs have entered development as patents on these more complex proteins expire. In September 2013, the first biosimilar mAb, infliximab, was authorised in Europe. In March 2015, the first biosimilar (Zarxio™, filgrastim-sndz, Sandoz) was approved by the US Food and Drug Administration; however, to date no mAb biosimilars have been approved in the US. There are currently major differences between how biosimilars are regulated in different parts of the world, leading to substantial variability in the amount of in vivo nonclinical toxicity testing required to support clinical development and marketing of biosimilars. There are approximately 30 national and international guidelines on biosimilar development and this number is growing. The European Union's guidance describes an approach that enables biosimilars to enter clinical trials based on robust in vitro data alone; in contrast, the World Health Organization's guidance is interpreted globally to mean in vivo toxicity studies are mandatory. We reviewed our own experience working in the global regulatory environment, surveyed current practice, determined drivers for nonclinical in vivo studies with biosimilar mAbs and shared data on practice and study design for 25 marketed and as yet unmarketed biosimilar mAbs that have been in development in the past 5y. These data showed a variety of nonclinical in vivo approaches, and also demonstrated the practical challenges faced in obtaining regulatory approval for clinical trials based on in vitro data alone. The majority of reasons for carrying out nonclinical in vivo studies were not based on scientific rationale, and therefore the authors have made recommendations for a data-driven approach to the toxicological assessment of mAb biosimilars that minimises unnecessary use of animals and can be used across all regions of the world. Taylor & Francis 2016-02-06 /pmc/articles/PMC4966840/ /pubmed/26854177 http://dx.doi.org/10.1080/19420862.2016.1145331 Text en © 2016 The Author(s). Published with license by Taylor & Francis Group, LLC http://creativecommons.org/licenses/by-nc/3.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-Non-Commercial License (http://creativecommons.org/licenses/by-nc/3.0/), which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited. The moral rights of the named author(s) have been asserted.
spellingShingle Perspective
Chapman, Kathryn
Adjei, Akosua
Baldrick, Paul
da Silva, Antonio
De Smet, Karen
DiCicco, Richard
Hong, Seung Suh
Jones, David
Leach, Michael W.
McBlane, James
Ragan, Ian
Reddy, Praveen
Stewart, Donald I. H.
Suitters, Amanda
Sims, Jennifer
Waiving in vivo studies for monoclonal antibody biosimilar development: National and global challenges
title Waiving in vivo studies for monoclonal antibody biosimilar development: National and global challenges
title_full Waiving in vivo studies for monoclonal antibody biosimilar development: National and global challenges
title_fullStr Waiving in vivo studies for monoclonal antibody biosimilar development: National and global challenges
title_full_unstemmed Waiving in vivo studies for monoclonal antibody biosimilar development: National and global challenges
title_short Waiving in vivo studies for monoclonal antibody biosimilar development: National and global challenges
title_sort waiving in vivo studies for monoclonal antibody biosimilar development: national and global challenges
topic Perspective
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4966840/
https://www.ncbi.nlm.nih.gov/pubmed/26854177
http://dx.doi.org/10.1080/19420862.2016.1145331
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