Abstract
BackgroundMany new cancer drugs are being approved by reputed regulatory authorities without evidence of overall survival benefit, quality of life improvement, and often based on clinical trials at high risk of bias. In recent years, most Latin American (LA) countries have reformed their marketing authorization (MA) rules to directly accept or abbreviate the approval process in case of earlier authorization by the European Medicines Agency (EMA) and the US Food and Drug Administration, mainly. This study assessed the potential impact of decisions taken by EMA regarding the approval of new cancer drugs based on no evidence of overall survival or in potentially biased clinical trials in LA countries.DesignDescriptive analysis.SettingPublicly accessible marketing authorization databases from LA regulators, European Public Assessment Report by EMA, and previous studies accessing EMA approvals of new cancer drugs 2009–2016.Main outcome and measuresNumber of new cancer drugs approved by LA countries without evidence of overall survival (2009–2013), and without at least one clinical trial scored at low risk of bias, or with no trial supporting the marketing authorization at all (2014–2016).ResultsArgentina, Brazil, Chile, Colombia, Ecuador, Panama and Peru have publicly accessible and trustful MA databases and were included. Of the 17 cancer drugs approved by EMA (2009–2013) without evidence of OS benefit after a postmarketing median time of 5.4 years, 6 LA regulators approved more than 70% of them. Of the 13 drugs approved by EMA (2014–2016), either without supporting trial or with no trial at low risk of bias, Brazil approved 11, Chile 10, Peru 10, Argentina 10, Colombia 9, Ecuador 9, and Panama 8.ConclusionsLA countries keep approving new cancer drugs often based on poorly performed clinical trials measuring surrogate endpoints. EMA and other reputed regulators must be aware that their regulatory decisions might directly influence decisions regarding MA, health budgets and patient’s care elsewhere.
Highlights
Regulatory authorities play a critical role to assure the entrance of effective and safe therapeutic products into the market
Of the 17 cancer drugs approved by European Medicines Agency (EMA) (2009–2013) without evidence of overall survival (OS) benefit after a postmarketing median time of 5.4 years, 6 Latin American (LA) regulators approved more than 70% of them
LA countries keep approving new cancer drugs often based on poorly performed clinical trials measuring surrogate endpoints
Summary
Regulatory authorities play a critical role to assure the entrance of effective and safe therapeutic products into the market. Regulatory decisions taken by European Medicines Agency (EMA) and US Food and Drug Administration (FDA) to approve new cancer drugs are often based on studies with no or disappointing results on primary clinical endpoints [3,4,5,6,7,8,9], and on methodologically doubtful clinical trials [10,11,12]. Many new cancer drugs are being approved by reputed regulatory authorities without evidence of overall survival benefit, quality of life improvement, and often based on clinical trials at high risk of bias. This study assessed the potential impact of decisions taken by EMA regarding the approval of new cancer drugs based on no evidence of overall survival or in potentially biased clinical trials in LA countries
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