Invest Radiol. 2018 Feb;53(2):70-79. doi: 10.1097/RLI.0000000000000412.
The primary objective of this study was to investigate the pharmacokinetic profile of gadoterate meglumine in pediatric patients younger than 2 years; the secondary objectives were to document its efficacy and safety.
This was a Phase IV open-label, prospective study conducted in 9 centers (4 countries). Forty-five patients younger than 2 years with normal estimated glomerular filtration rate and scheduled to undergo routine gadolinium-enhanced magnetic resonance imaging (MRI) of any organ were included and received a single intravenous injection of gadoterate meglumine (0.1 mmol/kg). To perform the population pharmacokinetics analysis, 3 blood samples per subject were drawn during 3 time windows at time points allocated by randomization.
Gadoterate meglumine concentrations were best fitted using a 2-compartmental model with linear elimination from central compartment. The median total clearance adjusted to body weight was estimated at 0.06 L/h per kg and increased with estimated glomerular filtration rate according to a power model. The median volume of distribution at steady state (Vss) adjusted to body weight was estimated at 0.047 L/kg. Estimated median terminal half-life (t1/2β) was 1.35 h, and the median systemic exposure (area under the curve) was 1591 μmol h/L. Efficacy was assessed by comparing precontrast +postcontrast images to precontrast images in a subset of 28 subjects who underwent an MRI examination of brain, spine, and associated tissues. A total of 28 lesions were identified and analyzed in 15 subjects with precontrast images versus 30 lesions in 16 subjects with precontrast + postcontrast images. Lesion visualization was improved with a mean (SD) increase in scores at subject level of 0.7 (1.0) for lesion border delineation, 0.9 (1.6) for internal morphology, and 3.1 (3.2) for contrast enhancement. Twenty-six adverse events occurred postinjection in 13 subjects (28.9%), including 3 serious reported in 1 subject (2.2%). One subject (2.2%) experienced 1 rash of moderate intensity considered as related to gadoterate meglumine.
The pharmacokinetic profile of gadoterate meglumine after a single intravenous injection of 0.1 mmol/kg was appropriately described in newborns and infants younger than 2 years, for whom no dose adjustment is required. The improved efficacy of gadoterate meglumine for contrast-enhanced MRI examination of brain, spine, and associated tissues, as well as its good safety profile, was also demonstrated in this population.
本研究的主要目的是研究 2 岁以下儿科患者中钆特酸葡胺的药代动力学特征;次要目的是记录其疗效和安全性。
这是一项在 9 个中心(4 个国家)进行的 IV 期、开放标签、前瞻性研究。45 名肾小球滤过率正常且计划接受任何器官常规钆增强磁共振成像(MRI)的 2 岁以下患者入选,并接受单次静脉注射钆特酸葡胺(0.1mmol/kg)。为了进行群体药代动力学分析,每个受试者在随机分配的时间点的 3 个时间窗内抽取 3 个血样。
钆特酸葡胺浓度最好用具有线性从中央室消除的 2 室模型拟合。根据幂模型,调整至体重的总清除率估计为 0.06L/h/kg,并随肾小球滤过率增加而增加。调整至体重的稳态分布容积(Vss)中位数估计为 0.047L/kg。估计的中位终末半衰期(t1/2β)为 1.35h,中位系统暴露量(曲线下面积)为 1591μmol h/L。通过比较 28 名接受脑、脊柱和相关组织 MRI 检查的受试者的对比前+对比后图像与对比前图像,评估疗效。在 15 名受试者中有 28 个病变的对比前图像与 16 名受试者中有 30 个病变的对比前+对比后图像中识别并分析了总共 28 个病变。病变可视化得到改善,病变边界描绘的平均(SD)受试者水平评分提高 0.7(1.0),内部形态提高 0.9(1.6),增强对比提高 3.1(3.2)。13 名受试者(28.9%)在注射后发生 26 次不良事件,其中 1 名受试者(2.2%)报告 1 例严重不良事件。1 名受试者(2.2%)出现 1 例中度强度皮疹,认为与钆特酸葡胺有关。
在 2 岁以下新生儿和婴儿中,单次静脉注射 0.1mmol/kg 后的钆特酸葡胺药代动力学特征得到了适当描述,无需调整剂量。在该人群中还证明了钆特酸葡胺用于脑、脊柱和相关组织增强 MRI 检查的疗效改善以及良好的安全性。
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