评估上市前因素以预测上市后黑框警告和安全性撤市情况。
Evaluation of Pre-marketing Factors to Predict Post-marketing Boxed Warnings and Safety Withdrawals.
作者信息
Schick Andreas, Miller Kathleen L, Lanthier Michael, Dal Pan Gerald, Nardinelli Clark
机构信息
Office of Program and Strategic Analysis, Center for Drug Evaluation and Research, U.S. Food and Drug Administration, 10903 New Hampshire Avenue, Silver Spring, MD, USA.
Office of Planning, Office of the Commissioner, U.S. Food and Drug Administration, 10903 New Hampshire Avenue, Silver Spring, MD, USA.
出版信息
Drug Saf. 2017 Jun;40(6):497-503. doi: 10.1007/s40264-017-0526-1.
INTRODUCTION
An important goal in drug regulation is understanding serious safety issues with new drugs as soon as possible. Achieving this goal requires us to understand whether information provided during the Food and Drug Administration (FDA) drug review can predict serious safety issues that are usually identified after the product is approved. However, research on this topic remains understudied. In this paper, we examine whether any pre-marketing drug characteristics are associated with serious post-marketing safety actions.
METHODS
We study this question using an internal FDA database containing every new small molecule drug submitted to the FDA's Center for Drug Evaluation and Research (CDER) on or after November 21, 1997, and approved and commercially launched before December 31, 2009. Serious post-marketing safety actions include whether these drugs ever experienced either a post-marketing boxed warning or a withdrawal from the market due to safety concerns. A random effects logistic regression model was used to test whether any pre-marketing characteristics were associated with either post-marketing safety action.
RESULTS
A total of 219 new molecular entities were analyzed. Among these drugs, 11 experienced a safety withdrawal and 30 received boxed warnings by July 31, 2016. Contrary to prevailing hypotheses, we find that neither clinical trial sample sizes nor review time windows are associated with the addition of a post-marketing boxed warning or safety withdrawal. However, we do find that new drugs approved with either a boxed warning or priority review are more likely to experience post-marketing boxed warnings. Furthermore, drugs approved with boxed warnings tend to receive post-marketing boxed warnings resulting from new safety information that are unrelated to the original warning. Drugs approved with a boxed warning are 3.88 times more likely to receive a post-marketing boxed warning, while drugs approved with a priority review are 3.51 times more likely to receive a post-marketing boxed warning.
CONCLUSION
Although drugs approved with a boxed warning or priority review are more likely to experience serious post-marketing safety events, other information provided during the FDA drug review that is easy to quantify is generally not associated with post-marketing safety events. It appears that these post-marketing events are not discernible during a pre-marketing review and therefore might not be avoidable using current review data.
引言
药品监管的一个重要目标是尽快了解新药的严重安全问题。要实现这一目标,我们需要了解美国食品药品监督管理局(FDA)药品审评过程中提供的信息是否能够预测通常在产品获批后才发现的严重安全问题。然而,关于这一主题的研究仍未得到充分探讨。在本文中,我们研究了是否有任何上市前药品特征与严重的上市后安全行动相关。
方法
我们使用FDA的一个内部数据库来研究这个问题,该数据库包含1997年11月21日及之后提交给FDA药品评价和研究中心(CDER)、并于2009年12月31日前获批并上市的每一种新型小分子药物。严重的上市后安全行动包括这些药物是否曾经历上市后黑框警告或因安全问题退市。我们使用随机效应逻辑回归模型来测试是否有任何上市前特征与上市后安全行动相关。
结果
总共分析了219个新分子实体。在这些药物中,截至2016年7月31日,有11种经历了安全退市,30种收到了黑框警告。与普遍的假设相反,我们发现临床试验样本量和审评时间窗口均与上市后黑框警告或安全退市无关。然而,我们确实发现,获批时带有黑框警告或优先审评的新药更有可能经历上市后黑框警告。此外,获批时带有黑框警告的药物往往会因与原始警告无关的新安全信息而收到上市后黑框警告。获批时带有黑框警告的药物收到上市后黑框警告的可能性是其他药物的3.88倍,而获批时经过优先审评的药物收到上市后黑框警告的可能性是其他药物的3.51倍。
结论
尽管获批时带有黑框警告或优先审评的药物更有可能经历严重的上市后安全事件,但FDA药品审评过程中提供的其他易于量化的信息通常与上市后安全事件无关。看来这些上市后事件在上市前审评期间是无法察觉的,因此使用当前的审评数据可能无法避免。
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