口服给予健康受试者后咪达非那新的绝对生物利用度。
Absolute bioavailability of imidafenacin after oral administration to healthy subjects.
作者信息
Ohno Tomoya, Nakade Susumu, Nakayama Kazuki, Kitagawa Junsaku, Ueda Shinya, Miyabe Hiroyuki, Masuda Yuichi, Miyata Yasuyuki
机构信息
Pharmacokinetic Research Laboratories, Ono Pharmaceutical Co., Ltd, Ibaraki, Japan.
出版信息
Br J Clin Pharmacol. 2008 Feb;65(2):197-202. doi: 10.1111/j.1365-2125.2007.02999.x.
WHAT IS ALREADY KNOWN ABOUT THIS SUBJECT
The absolute bioavailability of imidafenacin in rats and dogs is 5.6% and 36.1%, respectively. The pharmacokinetic profiles of imidafenacin after oral administration have been revealed. Imidafenacin is primarily metabolized to metabolites by CYP3A4 and UGT1A4.
WHAT THIS STUDY ADDS
The absolute bioavailability of imidafenacin in human is 57.8%. The pharmacokinetic profiles of imidafenacin after intravenous administration are revealed. The formation of metabolites in the plasma is caused mainly by first-pass effects.
AIMS
To investigate the absolute bioavailability of imidafenacin, a new muscarinic receptor antagonist, a single oral dose of 0.1 mg imidafenacin was compared with an intravenous (i.v.) infusion dose of 0.028 mg of the drug in healthy subjects.
METHODS
Fourteen healthy male subjects, aged 21-45 years, received a single oral dose of 0.1 mg imidafenacin or an i.v. infusion dose of 0.028 mg imidafenacin over 15 min at two treatment sessions separated by a 1-week wash-out period. Plasma concentrations of imidafenacin and the major metabolites M-2 and imidafenacin-N-glucuronide (N-Glu) were determined. The urinary excretion of imidafenacin was also evaluated. Analytes in biological samples were measured by liquid chromatography tandem mass spectrometry.
RESULTS
The absolute oral bioavailability of imidafenacin was 57.8% (95% confidence interval 54.1, 61.4) with a total clearance of 29.5 +/- 6.3 l h(-1). The steady-state volume of distribution was 122 +/- 28 l, suggesting that imidafenacin distributes to tissues. Renal clearance after i.v. infusion was 3.44 +/- 1.08 l h(-1), demonstrating that renal clearance plays only a minor role in the elimination of imidafenacin. The ratio of AUC(t) of both M-2 and N-Glu to that of imidafenacin was reduced after i.v. infusion from that seen after oral administration, suggesting that M-2 and N-Glu in plasma after oral administration were generated primarily due to first-pass metabolism. No serious adverse events were reported during the study.
CONCLUSIONS
The absolute mean oral bioavailability of imidafenacin was determined to be 57.8%. Imidafenacin was well tolerated following both oral administration and i.v. infusion.
关于该主题已知的信息
咪达非那新在大鼠和犬体内的绝对生物利用度分别为5.6%和36.1%。已揭示了咪达非那新口服给药后的药代动力学特征。咪达非那新主要通过CYP3A4和UGT1A4代谢为代谢产物。
本研究增加的内容
咪达非那新在人体内的绝对生物利用度为57.8%。揭示了咪达非那新静脉给药后的药代动力学特征。血浆中代谢产物的形成主要由首过效应引起。
目的
为研究新型毒蕈碱受体拮抗剂咪达非那新的绝对生物利用度,在健康受试者中比较了单次口服0.1 mg咪达非那新与静脉输注0.028 mg该药物的情况。
方法
14名年龄在21 - 45岁的健康男性受试者,在两个治疗周期中分别接受单次口服0.1 mg咪达非那新或在15分钟内静脉输注0.028 mg咪达非那新,两个周期之间有1周的洗脱期。测定了咪达非那新及其主要代谢产物M - 2和咪达非那新 - N - 葡萄糖醛酸苷(N - Glu)的血浆浓度。还评估了咪达非那新的尿排泄情况。生物样品中的分析物通过液相色谱串联质谱法测定。
结果
咪达非那新的绝对口服生物利用度为57.8%(95%置信区间54.1, 61.4),总清除率为29.5±6.3 l h⁻¹。稳态分布容积为(122±28)l,表明咪达非那新分布于组织中。静脉输注后的肾清除率为3.44±1.08 l h⁻¹,表明肾清除在咪达非那新的消除中仅起次要作用。静脉输注后M - 2和N - Glu的AUC(t)与咪达非那新的AUC(t)之比低于口服给药后的比值,表明口服给药后血浆中的M - 2和N - Glu主要是由首过代谢产生的。研究期间未报告严重不良事件。
结论
确定咪达非那新的绝对平均口服生物利用度为57.8%。咪达非那新口服给药和静脉输注后耐受性良好。
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