Bayer HealthCare Pharmaceutical, Schering Pharma AG, Global Medical Affairs Diagnostic Imaging, Berlin, Germany.
Invest Radiol. 2011 Nov;46(11):663-71. doi: 10.1097/RLI.0b013e3182218dc3.
To assess the clinical safety and tolerability of the macrocyclic contrast agent gadobutrol (Gadovist/Gadavist) overall and in specific patient populations based on clinical trials and postmarketing experience.
In total, 5545 patients enrolled in 34 prospective clinical studies were evaluated in an integrated analysis of safety. Of all enrolled patients, 4549 received gadobutrol at a dose of ≤ 0.09 mmol/kg body weight to a maximum of 0.51 mmol/kg body weight, with most patients (53.5%) receiving the recommended dose of >0.09 to 0.11 mmol/kg body weight. Data include comparisons with other extracellular contrast agents and subgroup analyses in pediatric patients, and patients with allergic disposition, renal impairment, hepatic impairment, or cardiovascular disease. Furthermore, worldwide postmarketing safety surveillance results, including nephrogenic systemic fibrosis reports, based on more than 5.7 million estimated applications are described.
One or more adverse events (AEs) assessed as related to the administration of gadobutrol were reported by 182 (4.0%) of the 4549 patients who participated in clinical trials. This is comparable to the incidence observed with the comparator contrast agents (74/1844 patients, 4.0%). The most common AEs, independent of drug relationship, were headache, nausea, feeling hot, and dysgeusia. The favorable safety profile of gadobutrol was also demonstrated in the following specific subpopulations in whom similar incidence rates were seen: pediatric patients aged 2 to 17 years (8/138 patients, 5.8%), patients with severe or moderate renal impairment (9/366 patients, 2.5%), patients with severe or moderate hepatic impairment (9/214 patients, 4.2%), and patients with cardiovascular disorders (42/1506 patients, 2.8%). Having been established in controlled clinical trials, this safety profile was also confirmed by postmarketing surveillance data. With more than 5.7 million estimated administrations of gadobutrol, a total of 1175 (0.02%) suspected adverse drug reactions have been reported. The most serious adverse reactions seen in postmarketing surveillance included rare reports of cardiac arrest, respiratory arrest, anaphylactoid shock, and nephrogenic systemic fibrosis. Incidence and type of AEs from postmarketing surveillance were consistent with the established safety profile.
The comprehensive analysis of safety data obtained from 34 clinical studies demonstrates that gadobutrol has an excellent safety profile and a positive benefit risk profile when used in patients in need of contrast-enhanced magnetic resonance imaging. Gadobutrol was well tolerated by adults, by children, by patients with impaired liver or kidney function, and by patients with cardiovascular disease. The favorable safety profile is confirmed by the available postmarketing surveillance data and is compared with that of other gadolinium-based contrast agents.
根据临床试验和上市后经验,评估大环造影剂钆布醇(加乐显/加乐显)的总体临床安全性和耐受性,以及特定患者人群中的安全性和耐受性。
在一项安全性综合分析中,共评估了 34 项前瞻性临床研究中 5545 名入组患者的安全性。在所有入组患者中,4549 名患者以≤0.09mmol/kg 体重的剂量接受了钆布醇治疗,最大剂量为 0.51mmol/kg 体重,大多数患者(53.5%)接受了推荐剂量>0.09 至 0.11mmol/kg 体重。数据包括与其他细胞外造影剂的比较以及儿科患者和过敏体质、肾功能损害、肝功能损害或心血管疾病患者的亚组分析。此外,还描述了基于超过 570 万次估计应用的全球上市后安全性监测结果,包括肾源性系统纤维化报告。
在参加临床试验的 4549 名患者中,有 182 名(4.0%)报告了 1 次或多次经评估与钆布醇给药相关的不良事件(AE)。这与比较造影剂(1844 名患者中的 74 名,4.0%)观察到的发生率相似。最常见的不良事件,与药物关系无关,为头痛、恶心、发热和味觉障碍。在以下特定亚组中,也显示了钆布醇有利的安全性特征,这些亚组的发生率相似:2 至 17 岁的儿科患者(138 名患者中的 8 名,5.8%)、严重或中度肾功能损害的患者(366 名患者中的 9 名,2.5%)、严重或中度肝功能损害的患者(214 名患者中的 9 名,4.2%)和心血管疾病患者(1506 名患者中的 42 名,2.8%)。在对照临床试验中已确定的安全性特征,也通过上市后监测数据得到证实。在超过 570 万次估计给药中,共报告了 1175 例(0.02%)可疑药物不良反应。上市后监测中最严重的不良反应包括罕见的心脏骤停、呼吸骤停、过敏性休克和肾源性系统纤维化的报告。上市后监测中不良事件的发生率和类型与既定的安全性特征一致。
34 项临床研究的安全性数据综合分析表明,在需要对比增强磁共振成像的患者中,钆布醇具有极好的安全性和积极的获益风险比。钆布醇在成人、儿童、肝肾功能损害患者以及心血管疾病患者中均具有良好的耐受性。现有的上市后监测数据证实了其良好的安全性特征,并与其他基于钆的造影剂进行了比较。
