患有严重先天性心脏病的新生儿在心脏手术与心肺旁路术前、术中和术后服用别嘌醇和羟嘌呤醇的群体药代动力学和目标值达标情况。

IF 4.6 2区 医学 Q1 PHARMACOLOGY & PHARMACY Clinical Pharmacokinetics Pub Date : 2024-08-01 Epub Date: 2024-08-15 DOI:10.1007/s40262-024-01401-3
Wan-Yu Chu, Maaike Nijman, Raymond Stegeman, Johannes M P J Breur, Nicolaas J G Jansen, Joppe Nijman, Kim van Loon, Erik Koomen, Karel Allegaert, Manon J N L Benders, Thomas P C Dorlo, Alwin D R Huitema
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引用次数: 0

摘要

背景:CRUCIAL试验(NCT04217421)正在研究出生后不久接受心肺旁路(CPB)心脏手术的危重先天性心脏病(CCHD)新生儿在出生后和围手术期服用别嘌醇对术后脑损伤的影响:本研究旨在描述别嘌呤醇和奥昔嘌呤醇在该人群术前、术中和术后阶段的药代动力学(PK)特征,并评估当前给药策略的目标达成情况:我们使用非线性混合效应模型为 CRUCIAL 试验中的 14 名新生儿建立了群体 PK 模型,这些新生儿在出生后和围手术期接受了多达五次的别嘌醇静脉注射。达到目标的定义是:在出生后的头 24 小时内以及在使用 CPB 进行心脏手术后的开始至 36 小时内,至少有三分之二的患者体内别嘌醇浓度大于 2 mg/L:将别嘌醇的二室模型与氧嘌呤醇的一室模型连接起来,后者在转换过程中具有自动抑制作用,能最好地描述PK。在出生后 5.6 天接受心脏手术的体重为 3.5 千克的典型新生儿中,出生时别嘌醇和奥昔嘌醇的清除率(CL)分别为 0.95 升/小时(95% 置信区间为 0.75-1.2)和 0.21 升/小时(0.17-0.27),随后随着 PNA 的增加,在 CPB 前分别为 2.97 升/小时和 0.41 升/小时。在 CPB 期间,别嘌醇和氧嘌呤醇的 CL 分别降至 1.38 升/小时(0.9-1.87)和 0.12 升/小时(0.05-0.22)。CPB 后,别嘌醇的 CL 升至 2.21 升/小时(1.74-2.83),而奥昔布洛尔的 CL 降至 0.05 升/小时(0.01-0.1)。产后 24 小时、CPB 开始后 24 小时和心脏手术结束后 36 小时的目标达标率分别为 100%、53.8% 和 100%。在整个出生后和围手术期,别嘌醇和氧嘌呤醇的联合浓度对黄嘌呤氧化酶的抑制率(IC90XO)均≥90%:在 CRUCIAL 试验中,别嘌醇的最小目标浓度并不是在每个预定的时间间隔内都能达到;但是,所采用的给药策略被认为是适当的,因为它所产生的浓度远远超过了 IC90XO。在 CPB 期间,两种化合物的 CL 均有所降低,这表明低体温、血液滤过和回路中可能存在的别嘌醇螯合作用都会产生影响。CPB 后氧嘌呤醇的 CL 值降低可能是由于肾功能受损所致。
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Population Pharmacokinetics and Target Attainment of Allopurinol and Oxypurinol Before, During, and After Cardiac Surgery with Cardiopulmonary Bypass in Neonates with Critical Congenital Heart Disease.

Background: The CRUCIAL trial (NCT04217421) is investigating the effect of postnatal and perioperative administration of allopurinol on postoperative brain injury in neonates with critical congenital heart disease (CCHD) undergoing cardiac surgery with cardiopulmonary bypass (CPB) shortly after birth.

Objective: This study aimed to characterize the pharmacokinetics (PK) of allopurinol and oxypurinol during the preoperative, intraoperative, and postoperative phases in this population, and to evaluate target attainment of the current dosing strategy.

Methods: Nonlinear mixed-effects modeling was used to develop population PK models in 14 neonates from the CRUCIAL trial who received up to five intravenous allopurinol administrations throughout the postnatal and perioperative periods. Target attainment was defined as achieving an allopurinol concentration >2 mg/L in at least two-thirds of the patients during the first 24 h after birth and between the start and 36 h after cardiac surgery with CPB.

Results: A two-compartment model for allopurinol was connected to a one-compartment model for oxypurinol with an auto-inhibition effect on the conversion, which best described the PK. In a typical neonate weighing 3.5 kg who underwent cardiac surgery at a postnatal age (PNA) of 5.6 days, the clearance (CL) of allopurinol and oxypurinol at birth was 0.95 L/h (95% confidence interval 0.75-1.2) and 0.21 L/h (0.17-0.27), respectively, which subsequently increased with PNA to 2.97 L/h and 0.41 L/h, respectively, before CPB. During CPB, allopurinol and oxypurinol CL decreased to 1.38 L/h (0.9-1.87) and 0.12 L/h (0.05-0.22), respectively. Post-CPB, allopurinol CL increased to 2.21 L/h (1.74-2.83), while oxypurinol CL dropped to 0.05 L/h (0.01-0.1). Target attainment was 100%, 53.8%, and 100% at 24 h postnatally, 24 h after the start of CPB, and 36 h after the end of cardiac surgery, respectively. The combined concentrations of allopurinol and oxypurinol maintained ≥ 90% inhibition of xanthine oxidase (IC90XO) throughout the postnatal and perioperative period.

Conclusions: The minimal target concentration of allopurinol was not achieved at every predefined time interval in the CRUCIAL trial; however, the dosing strategy used was deemed adequate, since it yielded concentrations well exceeding the IC90XO. The decreased CL of both compounds during CPB suggests influence of the hypothermia, hemofiltration, and the potential sequestration of allopurinol in the circuit. The reduced CL of oxypurinol after CPB is likely attributable to impaired kidney function.

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来源期刊
CiteScore
8.80
自引率
4.40%
发文量
86
审稿时长
6-12 weeks
期刊介绍: Clinical Pharmacokinetics promotes the continuing development of clinical pharmacokinetics and pharmacodynamics for the improvement of drug therapy, and for furthering postgraduate education in clinical pharmacology and therapeutics. Pharmacokinetics, the study of drug disposition in the body, is an integral part of drug development and rational use. Knowledge and application of pharmacokinetic principles leads to accelerated drug development, cost effective drug use and a reduced frequency of adverse effects and drug interactions.
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