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患者白细胞中磷酸化齐多夫定(ZDV)的浓度与ZDV剂量或血浆浓度无关。

Concentrations of phosphorylated zidovudine (ZDV) in patient leukocytes do not correlate with ZDV dose or plasma concentrations.

作者信息

Stretcher B N, Pesce A J, Murray J A, Hurtubise P E, Vine W H, Frame P T

机构信息

Department of Pathology, University of Cincinnati School of Medicine, Ohio.

出版信息

Ther Drug Monit. 1991 Jul;13(4):325-31. doi: 10.1097/00007691-199107000-00008.

DOI:10.1097/00007691-199107000-00008
PMID:1780965
Abstract

Zidovudine (ZDV) elicits its antiviral effect through intracellular metabolism to the 5'-triphosphate, which interferes with viral replication. Monitoring of the active metabolites of ZDV in cells could lead to an intracellular therapeutic range. This study was performed to determine whether a radioimmunoassay, previously used for in vitro quantitation of total phosphorylated ZDV inside peripheral blood leukocytes, could be used for similar determinations in patient samples. The relationship between ZDV dose, plasma concentrations, and intracellular metabolite concentrations was also examined. Ten-milliliter blood samples were drawn from each of 13 human immunodeficiency virus-infected patients and were assayed. Intracellular concentrations of phosphorylated ZDV ranged from 0.33 to 3.54 pmol/10(6) cells, similar to those observed in vitro. Phosphorylated ZDV was independent of dose, and did not correlate with plasma concentrations. Intracellular concentration in the patient population as a whole did not change during the 4-h dosing interval, while plasma concentration decayed normally. Later determinations in the same patients gave intracellular values within 31% of earlier values. Intraassay variability was less than 10%. Thus, the method is valid for measurement of phosphorylated ZDV in patient cells. Although individual concentrations showed no clear change during the 3-month study period, intracellular concentrations decreased with increasing length of therapy (up to 3 years) in the population as a whole. This suggests a decreased cellular ability to phosphorylate ZDV after prolonged exposure to drug. The lack of intracellular decay implies a half-life longer than the 1-h half-life of plasma ZDV. These data suggest that smaller doses or longer dosing intervals might maintain intracellular concentrations once steady state is achieved.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

齐多夫定(ZDV)通过在细胞内代谢为5'-三磷酸酯发挥抗病毒作用,该三磷酸酯可干扰病毒复制。监测细胞内ZDV的活性代谢产物可得出细胞内治疗范围。本研究旨在确定一种先前用于体外定量外周血白细胞内总磷酸化ZDV的放射免疫测定法是否可用于患者样本的类似测定。同时还研究了ZDV剂量、血浆浓度与细胞内代谢产物浓度之间的关系。从13名感染人类免疫缺陷病毒的患者中每人抽取10毫升血样进行检测。磷酸化ZDV的细胞内浓度范围为0.33至3.54 pmol/10(6)个细胞,与体外观察到的浓度相似。磷酸化ZDV与剂量无关,且与血浆浓度无相关性。在4小时给药间隔期间,整个人群的细胞内浓度没有变化,而血浆浓度正常衰减。对同一患者的后续测定得出的细胞内值在早期值的31%以内。批内变异小于10%。因此,该方法可有效测量患者细胞内的磷酸化ZDV。尽管在3个月的研究期间个体浓度没有明显变化,但总体人群中细胞内浓度随着治疗时间延长(长达3年)而降低。这表明长期接触药物后细胞磷酸化ZDV的能力下降。细胞内浓度没有衰减意味着其半衰期长于血浆ZDV的1小时半衰期。这些数据表明,一旦达到稳态,较小剂量或更长的给药间隔可能维持细胞内浓度。(摘要截断于250字)

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