8-甲氧基补骨脂素在人体静脉注射后的药代动力学。

The pharmacokinetics of 8-methoxypsoralen following i.v. administration in humans.

作者信息

Billard V, Gambus P L, Barr J, Minto C F, Corash L, Tessman J W, Stickney J L, Shafer S L

机构信息

Institut Gustave ROUSSY, Villejuif, France.

出版信息

Br J Clin Pharmacol. 1995 Oct;40(4):347-60. doi: 10.1111/j.1365-2125.1995.tb04557.x.

DOI:10.1111/j.1365-2125.1995.tb04557.x

PMID:8554937

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1365154/

Abstract

8-methoxypsoralen (8-MOP) is a naturally occurring photoreactive substance which, in the presence of u.v. light, forms covalent adducts with pyrimidine bases in nucleic acids. For many years, 8-MOP has been used in PUVA therapy for treatment of psoriasis. Recently, the drug has been found to inactivate effectively bacteria spiked into platelet concentrates. The purpose of this study was to determine the pharmacokinetics and safety of 8-MOP administered intravenously in the bactericidal dosage range. 2. Eighteen volunteers were divided into three treatment groups to receive, respectively, 5, 10, and 15 mg 8-MOP infused over 60 min. Frequent arterial samples were gathered, and the blood and plasma were assayed for 8-MOP concentration. The pharmacokinetic parameters were determined by moment and compartmental population analysis, the latter performed with the program NONMEM. Haemodynamics, ventilatory pattern, and subjective effects were recorded throughout the study. 3. The intravenously administered 8-MOP was well tolerated in all individuals, and no acute toxicity was observed. 4. The pharmacokinetics of 8-MOP were best described by a three-compartment mammillary model in which the volumes and clearances were proportional to weight. The mean pharmacokinetic parameters for the plasma concentrations were: V1 = 0.045 1 kg-1, V2 = 0.57 1 kg-1, V3 = 0.15 1 kg-1, CL1 (systemic) = 0.010 1 kg-1 min-1, CL2 = 0.0067 1 kg-1 min-1, CL3 = 0.012 1 kg-1 min-1. The mean pharmacokinetic parameters for the blood concentrations were: V1 = 0.061 1 kg-1, V2 = 1.15 1 kg-1, V3 = 0.21 1 kg-1, CL1 (systemic) = 0.015 1 kg-1 min-1, CL2 = 0.011 1 kg-1 min-1 and CL3 = 0.015 1 kg-1 min-1. 5. The plasma pharmacokinetic model described the observations with a median absolute error of 17%, and the blood pharmacokinetic model described the observations with a median absolute error of 18%. Analysis of the relative concentration of 8-MOP between plasma and red blood cells suggested concentration-dependent partitioning. 6. The addition of 7.5 mg 8-MOP to 300 ml platelet concentrate would produce bactericidal concentrations of 25 micrograms ml-1. Simulations based upon our data show that intravenous administration of 7.5 mg over 60 min would result in systemic concentrations of 8-MOP similar to those observed with conventional PUVA therapy. We conclude that the extensive safety history established in PUVA therapy will be applicable to this new application of 8-MOP.

摘要

8-甲氧基补骨脂素（8-MOP）是一种天然存在的光反应性物质，在紫外线照射下，它会与核酸中的嘧啶碱基形成共价加合物。多年来，8-MOP一直用于光化学疗法（PUVA）治疗银屑病。最近，人们发现该药物能有效灭活添加到血小板浓缩物中的细菌。本研究的目的是确定在杀菌剂量范围内静脉注射8-MOP的药代动力学和安全性。2. 18名志愿者被分为三个治疗组，分别接受5、10和15毫克的8-MOP，在60分钟内输注完毕。频繁采集动脉血样，检测血液和血浆中的8-MOP浓度。通过矩量法和房室群体分析法确定药代动力学参数，后者使用NONMEM程序进行。在整个研究过程中记录血流动力学、通气模式和主观效应。3. 静脉注射8-MOP在所有个体中耐受性良好，未观察到急性毒性。4. 8-MOP的药代动力学最好用三室乳头模型描述，其中容积和清除率与体重成正比。血浆浓度的平均药代动力学参数为：V1 = 0.045升/千克，V2 = 0.57升/千克，V3 = 0.15升/千克，CL1（全身）= 0.010升/千克·分钟，CL2 = 0.0067升/千克·分钟，CL3 = 0.012升/千克·分钟。血液浓度的平均药代动力学参数为：V1 = 0.061升/千克，V2 = 1.15升/千克，V3 = 0.21升/千克，CL1（全身）= 0.015升/千克·分钟，CL2 = 0.011升/千克·分钟，CL3 = 0.015升/千克·分钟。5. 血浆药代动力学模型描述观察结果的中位数绝对误差为17%，血液药代动力学模型描述观察结果的中位数绝对误差为18%。对血浆和红细胞中8-MOP相对浓度的分析表明存在浓度依赖性分配。6. 在300毫升血小板浓缩物中添加7.5毫克8-MOP将产生25微克/毫升的杀菌浓度。根据我们的数据进行的模拟表明，在60分钟内静脉注射7.5毫克8-MOP将导致8-MOP的全身浓度与传统PUVA疗法观察到的浓度相似。我们得出结论，PUVA疗法中确立的广泛安全记录将适用于8-MOP的这种新应用。