Cancer remains a leading cause of global mortality, increasing demand for effective and accessible therapies. Regulatory agencies are central to evaluating and approving new oncological technologies. To compare oncology drug approvals by the FDA, EMA, and ANVISA from 2020 to 2024, analyzing regulatory timelines, innovation profiles, therapeutic trends, and the interval between approval and incorporation into Brazil's Unified Health System (SUS). A retrospective study was conducted using publicly available data from the FDA, EMA, ANVISA, and the National Commission for Health Technology Incorporation (CONITEC). All first-time oncology drug approvals during the period were included. Approval dates, developer origin, exclusivity status, and time to potential SUS incorporation were assessed. The FDA granted 73 approvals, followed by the EMA (56) and ANVISA (18). Regulatory convergence was high between the FDA and EMA, whereas ANVISA showed median approval delays of 353 days compared with the FDA and 336 days compared with the EMA. Relatively balanced distribution between biological and synthetic medicines was observed, with approvals concentrated among US-headquartered companies and primarily indicated for lung cancer, multiple myeloma, and breast cancer. FDA and EMA decisions relied on a more heterogeneous mix of trial phases and designs, whereas ANVISA more frequently required phase 3 randomized studies. Incorporation into SUS remained limited. Greater integration between regulatory evaluation and health technology assessment is needed to reduce asymmetries and improve timely access to oncological innovations within SUS. Differences in oncology drug approvals across regulatory agencies contribute to delays in access to innovative cancer therapies in Brazil. Strengthening regulatory alignment and integration with health technology assessment may improve timely and equitable access within SUS. • The U.S. led global oncology approvals, with 73 FDA authorizations. • ANVISA showed significant approval delays versus FDA and EMA. • Patient access in Brazil was further limited by HTA delays and non-incorporation into SUS. • FDA and EMA decisions showed high convergence in pivotal evidence. • ANVISA relied more on phase 3 and randomized trials than FDA and EMA.
Silva et al. (Fri,) studied this question.
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