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植入新生儿动脉导管的西罗莫司洗脱支架的药代动力学

Pharmacokinetics of sirolimus-eluting stents implanted in the neonatal arterial duct.

作者信息

Lee Kyong-Jin, Seto Winnie, Benson Lee, Chaturvedi Rajiv R

机构信息

From The Labatt Family Heart Centre, Division of Cardiology (K.-J.L., L.B., R.R.C.) and the Department of Pharmacy (W.S.), The Hospital for Sick Children, University of Toronto School of Medicine, Toronto, Canada.

出版信息

Circ Cardiovasc Interv. 2015 May;8(5). doi: 10.1161/CIRCINTERVENTIONS.114.002233.

Abstract

BACKGROUND

Sirolimus-eluting stents may have clinical advantages over bare-metal stents in the extremely proliferative environment of the neonatal arterial duct. However, sirolimus has immunosuppressive actions and little is known regarding sirolimus pharmacokinetics in the newborn.

METHODS AND RESULTS

This is a retrospective review of sirolimus pharmacokinetics in neonates who underwent sirolimus-eluting stent implantation in the arterial duct for pulmonary blood flow augmentation. Pharmacokinetic parameters were obtained by noncompartmental analysis and by a Bayesian one-compartment nonlinear mixed model. Nine neonates received a single sirolimus-eluting stent with a total sirolimus dose of 245 μg (n = 1), 194 μg (n = 5), or 143 μg (n = 3). Peak sirolimus concentrations were 13.6 ± 4.5 μg/L (24.8 μg/L highest) and clearance was 0.042 ± 0.03 L/hour (noncompartmental analysis) and 0.051 L/hour (95% credible intervals 0.037-0.069, nonlinear mixed model). Sirolimus remained > 5 μg/L, the trough level used in oral immunosuppressive therapy, for (95% credible interval) 15.9 (11.4, 22.8), 12.9 (7.6, 19.0), and 8.4 (2.3, 14.5) days for the 245, 194, and 143 μg sirolimus dose stents, respectively. Estimates of the duration of systemic immunosuppression are provided for combinations of 2 stents.

CONCLUSIONS

In neonates after sirolimus-eluting stent implantation, peak sirolimus levels were 20 × higher and clearance 30 × lower than previously reported in older children and adults. Sirolimus levels were within the immunosuppressive range for a prolonged period, but with no observable clinically significant adverse outcomes.

摘要

背景

在新生儿动脉导管的极度增殖环境中,西罗莫司洗脱支架可能比裸金属支架具有临床优势。然而,西罗莫司具有免疫抑制作用,关于新生儿中西罗莫司的药代动力学知之甚少。

方法与结果

这是一项对在动脉导管中植入西罗莫司洗脱支架以增加肺血流量的新生儿的西罗莫司药代动力学的回顾性研究。通过非房室分析和贝叶斯单室非线性混合模型获得药代动力学参数。9名新生儿接受了单个西罗莫司洗脱支架,西罗莫司总剂量为245μg(n = 1)、194μg(n = 5)或143μg(n = 3)。西罗莫司峰值浓度为13.6±4.5μg/L(最高24.8μg/L),清除率为0.042±0.03L/小时(非房室分析)和0.051L/小时(95%可信区间0.037 - 0.069,非线性混合模型)。对于245μg、194μg和143μg西罗莫司剂量的支架,西罗莫司水平分别在口服免疫抑制治疗中使用的谷值水平(>5μg/L)以上持续(95%可信区间)15.9(11.4,22.8)天、12.9(7.6,19.0)天和8.4(2.3,14.5)天。还提供了2个支架组合的全身免疫抑制持续时间的估计值。

结论

在植入西罗莫司洗脱支架后的新生儿中,西罗莫司峰值水平比先前报道的大龄儿童和成人高20倍,清除率低30倍。西罗莫司水平在免疫抑制范围内持续较长时间,但未观察到明显的临床显著不良后果。

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