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Abstract
The purpose of this report was to review issues associated with the introduction of
alternative versions of biosimilars used in the oncology setting.
Data were obtained by searches of MEDLINE, PubMed, references from relevant English-language
articles, and guidelines from the European Medicines Agency.
When biosimilars are approved in EU, they will be considered 'comparable' to the reference
product, but this does not ensure therapeutic equivalence. Inherent differences between
biosimilars may produce dissimilarities in clinical efficacy, safety, and immunogenicity.
Switching biosimilars should be considered a change in clinical management. Regulatory
guidelines have been established for some biosimilar categories but, because of the
limited clinical experience with biosimilars at approval, pharmacovigilance programs
will be important to establish clinical databases. Guidelines also provide a mechanism
for the extrapolation of clinical indications (approved indications for which the
biosimilar has not been studied). This may be of concern where differences in biological
activity can result in adverse outcomes or when safety is paramount (e.g. stem cell
mobilization in healthy donors). These issues should be addressed in biosimilar labeling.
Biosimilars should provide cost savings and greater accessibility to biopharmaceuticals.
A thorough knowledge surrounding biosimilars will ensure the appropriate use of biopharmaceuticals.