皮下 C1 抑制剂用于预防遗传性血管性水肿患者发作的群体药代动力学研究。
Population pharmacokinetics of subcutaneous C1-inhibitor for prevention of attacks in patients with hereditary angioedema.
机构信息
CSL Behring, King of Prussia, Pennsylvania.
Department of Medicine, University of California San Diego and San Diego VA Healthcare, La Jolla, California.
出版信息
Clin Exp Allergy. 2018 Oct;48(10):1325-1332. doi: 10.1111/cea.13220. Epub 2018 Aug 26.
BACKGROUND
Long-term prophylaxis with subcutaneous (SC) administration of a highly concentrated plasma-derived C1-esterase inhibitor (C1-INH) formulation was recently approved by the Food and Drug Administration for hereditary angioedema (HAE) attack prevention.
OBJECTIVE
To characterize the population pharmacokinetics of C1-INH (SC) (HAEGARDA ; CSL Behring) in healthy volunteers and HAE patients, and assess the variability and influence of covariates on pharmacokinetics.
METHODS
C1-INH functional activity data obtained after administration of various C1-INH (intravenous; IV) and C1-INH (SC) doses from 1 study in healthy volunteers (n = 16) and 2 studies in subjects with HAE (n = 108) were pooled to develop a population pharmacokinetic model (NONMEM v7.2). Pharmacokinetic parameters derived from steady-state simulations based on the final model were also evaluated.
RESULTS
C1-INH functional activity following C1-INH (SC) administration was described by a linear one-compartment model with first-order absorption and elimination, with inter-individual variability in all parameters tested. The mean population bioavailability of C1-INH (SC), and pharmacokinetic parameters for clearance (CL), volume of distribution, and absorption rate were estimated to be 43%, 1.03 mL/hour/kg, 0.05 L/kg and 0.0146 hour , respectively. The effect of bodyweight on CL of C1-INH functional activity was included in the final model, estimated to be 0.74. Steady-state simulations of C1-INH functional activity vs time profiles in 1000 virtual HAE patients revealed higher minimum functional activity (C ) levels after twice-weekly dosing with 40 IU/kg (40%) and 60 IU/kg (48%) compared with 1000 IU IV (30%). Based on the population pharmacokinetic model, the median time to peak concentration was ~59 hours and the median apparent plasma half-life was ~69 hours.
CONCLUSIONS AND CLINICAL RELEVANCE
Twice-weekly bodyweight-adjusted dosing of C1-INH (SC) exhibits linear pharmacokinetics and dose-dependent increases in C levels at each dosing interval. In this analysis, SC dosing led to maintenance of higher C levels than IV dosing.
背景
最近,美国食品和药物管理局批准了皮下(SC)给予高度浓缩血浆衍生 C1-酯酶抑制剂(C1-INH)制剂用于遗传性血管性水肿(HAE)发作预防的长期预防。
目的
描述健康志愿者和 HAE 患者中 C1-INH(SC)(HAEGARDA;CSL Behring)的群体药代动力学特征,并评估变异性和协变量对药代动力学的影响。
方法
从一项健康志愿者(n=16)和两项 HAE 受试者(n=108)的 1 项研究中,汇集了 C1-INH(静脉内;IV)和 C1-INH(SC)不同剂量给药后获得的 C1-INH 功能活性数据,以建立群体药代动力学模型(NONMEM v7.2)。还评估了基于最终模型的稳态模拟得出的药代动力学参数。
结果
C1-INH(SC)给药后 C1-INH 功能活性采用线性单室模型描述,具有一级吸收和消除,所有测试参数的个体间变异性。C1-INH(SC)的群体生物利用度、清除率(CL)、分布容积和吸收速率的药代动力学参数估计值分别为约 43%、1.03 mL/hour/kg、0.05 L/kg 和 0.0146 小时。体重对 C1-INH 功能活性 CL 的影响被包含在最终模型中,估计值为 0.74。在 1000 名虚拟 HAE 患者的 C1-INH 功能活性与时间的稳态模拟中,与 1000 IU IV 相比(30%),40 IU/kg(40%)和 60 IU/kg(~48%)的两周一次给药后,C 水平的最低功能活性(C )水平更高。基于群体药代动力学模型,达峰时间的中位数约为 59 小时,表观血浆半衰期的中位数约为 69 小时。
结论和临床意义
根据体重调整剂量的 C1-INH(SC)每周两次给药表现出线性药代动力学特征,并且在每个给药间隔内 C 水平的剂量依赖性增加。在这项分析中,SC 给药导致比 IV 给药维持更高的 C 水平。
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