Chien J Y, Banfield C R, Brazzell R K, Mayer P R, Slattery J T
Department of Pharmaceutics, University of Washington, Seattle 98195.
Pharm Res. 1992 Apr;9(4):469-73. doi: 10.1023/a:1015880011131.
To investigate the hypothesis that the pharmacokinetics of imirestat, an aldose reductase inhibitor, are influenced by saturable binding to tissues, three experiments were done. (1) The nature of the dose dependence was characterized in rats. Two groups of nine adult male Sprague-Dawley rats received iv 14C-imirestat at doses of 2 or 8 mg/kg. Serial blood samples were obtained over 15 days. Volume of distribution at steady-state was significantly different between the high- and the low-dose groups (0.744 +/- 0.103 l and 1.10 +/- 0.228 L, respectively). Clearance was independent of dose over this fourfold range (approximately 15 ml/hr). (2) The effect of either statil or AL3152, both aldose reductase inhibitors and potential competitors for aldose reductase binding, on the pharmacokinetics of a single 0.2-mg/kg iv dose of imirestat was assessed. A 2.4-mg/kg loading dose of statil was administered and a constant-rate infusion (56 micrograms/hr/kg) was begun 16 hr before imirestat. A 2-mg/kg loading dose of AL3152 and a constant-rate infusion (115 micrograms/kg/hr) were also administered 16 hr before imirestat. The infusions were maintained throughout the study. AL3152 administration decreased the imirestat steady-state volume of distribution by a mean of 63%. Statil administration decreased it by a mean of 39%. (3) The dosing regimen of the second study was repeated and, at two sampling times, nine tissues and plasma were obtained from four rats per sampling time for determination of imirestat tissue-to-plasma concentration ratio. The tissue/plasma imirestat concentration ratio in the adrenals 24 hr after imirestat administration was 56.9 +/- 20.0 in the imirestat group, 17.7 +/- 1.27 in the statil-coadministered group, and 12.3 +/- 2.59 in the AL3152-coadministered group.(ABSTRACT TRUNCATED AT 250 WORDS)
为了研究醛糖还原酶抑制剂依米司他的药代动力学是否受其与组织的饱和性结合影响,进行了三项实验。(1)在大鼠中表征剂量依赖性的性质。两组各9只成年雄性Sprague-Dawley大鼠分别静脉注射2或8mg/kg的14C-依米司他。在15天内采集系列血样。高剂量组和低剂量组的稳态分布容积显著不同(分别为0.744±0.103L和1.10±0.228L)。在此四倍剂量范围内清除率与剂量无关(约15ml/hr)。(2)评估醛糖还原酶抑制剂他汀或AL3152(二者均为醛糖还原酶抑制剂且是醛糖还原酶结合的潜在竞争者)对单次静脉注射0.2mg/kg依米司他药代动力学的影响。给予2.4mg/kg的他汀负荷剂量,并在依米司他给药前16小时开始恒速输注(56μg/hr/kg)。在依米司他给药前16小时还给予2mg/kg的AL3152负荷剂量和恒速输注(115μg/kg/hr)。在整个研究过程中维持输注。给予AL3152使依米司他的稳态分布容积平均降低63%。给予他汀使其平均降低39%。(3)重复第二项研究的给药方案,并且在两个采样时间点,每个采样时间从4只大鼠获取9种组织和血浆以测定依米司他的组织与血浆浓度比。依米司他给药24小时后,依米司他组肾上腺中的组织/血浆依米司他浓度比为56.9±20.0,他汀共同给药组为17.7±1.27,AL3152共同给药组为12.3±2.59。(摘要截断于250字)
