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Adverse immunostimulation caused by impurities: The dark side of biopharmaceuticals. | LitMetric

AI Article Synopsis

  • - Drug safety, particularly during the experimental development of biopharmaceuticals, is crucial due to risks like adverse immunostimulation (AI), which can lead to severe inflammatory reactions.
  • - Impurities from microbial sources in biopharmaceuticals can cause AI, highlighting flaws in current quality control and safety testing guidelines that do not adequately address these issues.
  • - The international guidelines lack recommendations for testing immunotoxicity and fail to account for other harmful impurities, making it important to share case studies of AI to improve awareness and future prevention strategies.

Article Abstract

Drug safety is an important issue, especially in the experimental phases of development. Adverse immunostimulation (AI) is sometimes encountered following treatment with biopharmaceuticals, which can be life-threatening if it results in a severe systemic inflammatory reaction. Biopharmaceuticals that unexpectedly induce an inflammatory response still enter the clinic, even while meeting all regulatory requirements. Impurities (of microbial origin) in biopharmaceuticals are an often-overlooked cause of AI. This demonstrates that the current guidelines for quality control and safety pharmacology testing are not flawless. Here, based on two case examples, several shortcomings of the guidelines are discussed. The most important of these are the lack of sensitivity for impurities, lack of testing for pyrogens other than endotoxin, and the use of insensitive animal species and biomarkers in preclinical investigations. Moreover, testing for the immunotoxicity of biopharmaceuticals is explicitly not recommended by the international guidelines. Publication of cases of AI is pivotal, both to increase awareness and to facilitate scientific discussions on how to prevent AI in the future.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6595286PMC
http://dx.doi.org/10.1111/bcp.13938DOI Listing

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