School of Pharmacy, University of Georgia, Athens, GA, USA.
MAbs. 2012 May-Jun;4(3):392-7. doi: 10.4161/mabs.19895. Epub 2012 Apr 26.
Monoclonal antibodies (mAbs) are known to cause hypersensitivity reactions (HSRs). The reactions pose a significant challenge to investigators, regulators, and health providers. Because HSRs cannot be predicted through the pharmacological basis of a therapy, clinical data are often relied upon to detect the reactions. Unfortunately, clinical studies are often unable to adequately characterize HSRs especially in therapies for orphan diseases. HSRs can go undetected until post-marketing safety surveillance when a large number of patients have been exposed to the therapy. The presented data demonstrates how hypersensitivity reaction warnings have changed over time in the prescribing information (PI), i.e., the drug package insert, through August 1, 2011 for 28 US-marketed mAbs. Tracking all PI revisions for each mAb over time revealed that hypersensitivity warning statements were expanded to include more severe manifestations. Over the course of a mAb therapy's life cycle, the hypersensitivity warning is twice more likely to be upgraded than downgraded in priority. Approximately 85% of hypersensitivity-associated fatality warnings were added in PI revisions as a result of post-marketing experience. Over 60% (20/33) of revisions to hypersensitivity warnings occurred within 3-4 y of product approval. While HSRs are generally recognized and described in the initial PI of mAbs, fatal HSRs are most commonly observed in post-marketing surveillance. Results of this study suggest that initial product labeling information may not describe rare but clinically significant occurrences of severe or fatal HSRs, but subsequent label revisions include rare events observed during post-marketed product use.
单克隆抗体(mAbs)已知会引起过敏反应(HSRs)。这些反应给研究人员、监管机构和医疗保健提供者带来了重大挑战。由于 HSR 不能通过治疗的药理学基础来预测,因此通常依赖临床数据来检测这些反应。不幸的是,临床研究往往无法充分描述 HSR,尤其是在孤儿病的治疗中。HSR 可能在上市后安全监测中才被发现,此时大量患者已经接触到了这种治疗。所呈现的数据展示了 2011 年 8 月 1 日之前,28 种美国市场销售的 mAbs 在处方信息(PI)中,即药物说明书中,过敏反应警告是如何随时间变化的。跟踪每个 mAb 的所有 PI 修订版可以发现,过敏警告声明被扩展到包括更严重的表现。在 mAb 治疗的生命周期中,过敏警告的优先级升级的可能性是降级的两倍。由于上市后经验,约 85%的与过敏相关的致死警告是在 PI 修订版中添加的。超过 60%(20/33)的过敏警告修订版是在产品批准后 3-4 年内进行的。虽然 HSR 通常在 mAbs 的初始 PI 中得到识别和描述,但致命的 HSR 最常见于上市后监测中。这项研究的结果表明,初始产品标签信息可能无法描述罕见但具有临床意义的严重或致命 HSR 事件,但随后的标签修订版包括在上市后产品使用过程中观察到的罕见事件。