FDA Publish Guidance on Interpreting Reproductive and Development Toxicities Reports
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This guidance describes an approach to estimating possible human developmental or reproductive risks associated with drug or biological product exposure when a nonclinical finding of toxicity has been identified, but definitive human data are unavailable. The guidance is intended for applicants of new drug applications (NDAs) and biologics licensing applications (BLAs). The recommendations included here will also help to ensure a consistent review of reproductive and developmental toxicity data among Center for Drug Evaluation and Research (CDER) review staff.
This guidance does not (1) give detailed advice about labeling or placement of toxicity information in product labeling (for information on labeling, see 21 CFR 201.57); or (2) discuss clinical data or the integration of nonclinical and clinical data.
The approach presented here for assessing nonclinical reproductive and developmental toxicity data involves the integration and careful consideration of a variety of different types of nonclinical information: reproductive toxicology; general toxicology; and toxicokinetic and pharmacokinetic information, including absorption, distribution, metabolism, and elimination data. The approach is used when there is a toxicity finding and focuses on assessing the likelihood that a drug will increase the risk of adverse human developmental or reproductive outcomes. The approach includes noting when studies were not conducted or when they were not performed using relevant model systems or at appropriate dose ranges. The general principles described here (i.e., a comprehensive analysis of available data) will typically be relevant to both drug and biological products, although some factors may not apply to biological products, because data may not be available for all factors considered in this guidance (e.g., cross-species concordance, dose-response, metabolism, relative exposure (animal : human) of >25-fold). For some oncology products (e.g., cytotoxics), certain aspects of the guidance may not apply because patients may be dosed at the maximum tolerated dose (MTD). Note: Available clinical information to evaluate a drug’s potential to increase the risk of an adverse developmental or reproductive outcome in humans should be evaluated separately and, when definitive, can supersede any nonclinical findings.
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