吉妥单抗奥佐米星相关肝窦阻塞综合征的评估:来自学术性药物警戒项目审查及药企赞助登记处的结果
Evaluation of gemtuzumab ozogamycin associated sinusoidal obstructive syndrome: Findings from an academic pharmacovigilance program review and a pharmaceutical sponsored registry.
作者信息
Magwood-Golston Jametta S, Kessler Samuel, Bennett Charles L
机构信息
Southern Network on Adverse Reactions (SONAR), South Carolina Center of Economic Excellence for Medication Safety, College of Pharmacy, University of South Carolina, Columbia, SC 29208, United States.
Southern Network on Adverse Reactions (SONAR), South Carolina Center of Economic Excellence for Medication Safety, College of Pharmacy, University of South Carolina, Columbia, SC 29208, United States.
出版信息
Leuk Res. 2016 May;44:61-4. doi: 10.1016/j.leukres.2016.03.004. Epub 2016 Mar 16.
BACKGROUND
In 2000, the Food and Drug Administration (FDA) approved gemtuzumab ozogamycin for monotherapy for older patients with relapsed AML. A 0.9% rate of hepatic sinusoidal obstructive syndrome (SOS) was noted in licensing trials. In 2001, FDA received reports of 14 GO-associated SOS cases from MD Anderson Cancer Center. A State of South Carolina/National Cancer Institute funded pharmacovigilance program and a manufacturer sponsored registry independently evaluated this concern.
METHODS
The manufacturer's registry and the academic program focused on risk factors and incidence of GO-associated SOS in routine clinical practice and clinical trial settings, respectively. Comparisons were made of findings and dissemination efforts from the two studies.
RESULTS
Retrospective analysis of clinical trials by the academic initiative identified 99 cases of SOS among 221 GO-treated stem cell patients and 649 patients who did not undergo HSCTs. SOS rates were 3% when GO was administered at doses ≤6 mg/m(2) as monotherapy or with non-hepatotoxic agents; 28% when administered with 6-thioguanine, a hepatotoxic agent; 15% when administered as monotherapy at doses at a dose of 9 mg/m(2), and between 15% and 40% if a stem cell transplant (SCT) was performed within 3 months of GO administration. Death from SOS occurred in 33% of the cases. The manufacturer's registry prospectively evaluated 482 GO-treated patients who received a mean dose of 7.8 mg/m(2). Overall, 41% received concomitant chemotherapy, 18% had undergone prior SCT, 9.1% developed SOS, and death from SOS occurred in 60% of the SOS cases. Findings from each initiative were disseminated at national conferences and in peer-reviewed manuscripts beginning in 2003.
CONCLUSION
Retrospective review of clinical trials, case series, and FDA reports and prospective registries can provide important information on safety signals initially identified in licensing trials.
背景
2000年,美国食品药品监督管理局(FDA)批准吉妥单抗奥佐米星用于老年复发急性髓系白血病(AML)患者的单药治疗。在上市试验中观察到肝窦阻塞综合征(SOS)的发生率为0.9%。2001年,FDA收到来自MD安德森癌症中心的14例与吉妥单抗奥佐米星相关的SOS病例报告。南卡罗来纳州/国家癌症研究所资助的药物警戒项目和制造商发起的登记处分别独立评估了这一问题。
方法
制造商的登记处和学术项目分别关注常规临床实践和临床试验环境中与吉妥单抗奥佐米星相关的SOS的危险因素和发生率。对两项研究的结果和传播努力进行了比较。
结果
学术项目对临床试验的回顾性分析在221例接受吉妥单抗奥佐米星治疗的干细胞患者和649例未接受造血干细胞移植(HSCT)的患者中确定了99例SOS病例。当吉妥单抗奥佐米星以≤6mg/m²的剂量作为单药治疗或与非肝毒性药物联合使用时,SOS发生率为3%;与肝毒性药物6-硫鸟嘌呤联合使用时为28%;以9mg/m²的剂量单药治疗时为15%,如果在吉妥单抗奥佐米星给药后3个月内进行干细胞移植(SCT),则发生率在15%至40%之间。33%的病例死于SOS。制造商的登记处对482例接受吉妥单抗奥佐米星治疗的患者进行了前瞻性评估,这些患者的平均剂量为7.8mg/m²。总体而言,41%的患者接受了联合化疗,18%的患者曾接受过SCT,9.1%的患者发生了SOS,60%的SOS病例死于SOS。从2003年开始,每项研究的结果都在全国会议和同行评审的手稿中进行了传播。
结论
对临床试验、病例系列、FDA报告和前瞻性登记处的回顾性审查可以提供关于在上市试验中最初发现的安全信号的重要信息。
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