Ahr H J, Krause H P, Siefert H M, Suwelack D, Weber H
Institute of Pharmacokinetics, Bayer AG, Wuppertal, Fed. Rep. of Germany.
Arzneimittelforschung. 1988 Aug;38(8):1093-8.
The absorption, disposition and excretion of (+/-) 3-isobutyl-5-methyl 1,4-dihydro-2,6-dimethyl-4-(2-nitrophenyl)-pyridine-3,5-dicarboxylate (nisoldipine, Bay k 5552) have been studied following a single administration of the 14C-labelled compound to rats, dogs, monkey and swine via different routes (intravenous, oral, intraduodenal) in the dose range of 0.05-10 mg.kg-1. [14C]nisoldipine was absorbed rapidly and almost completely. Peak concentrations of radioactivity in plasma were reached 0.9 h (rat), 1.4 h (dog), and 3.6 h (monkey) after oral administration with normalized maximum concentrations being in the same range for all three species (0.49-0.79). The radioactivity was eliminated from plasma with half-lives between 42 h and 54 h within an observation period up to 3 days. The contribution of unchanged [14C]nisoldipine to the concentration of total radioactivity in plasma was low after oral administration (between 0.5% (monkey) and 3.4% (dog) in the peak) indicating an extensive presystemic elimination of this compound. The bioavailability was estimated at 3.4% in rats and 11.7% in dogs. [14C]nisoldipine was highly bound to plasma proteins with free fractions of 0.9-2.9%. The excretion of the radioactivity via urine and feces/bile both after oral and intravenous administration of [14C]nisoldipine occurred rapidly and almost completely within 48 h in all species. Very small residues in the body were recovered at the end of the experiments in rats and dogs (less than 1.6% of the dose). The biliary/fecal route of excretion was preferred in rats, dogs and swine, whereas in monkey 76% of the dose was excreted renally.(ABSTRACT TRUNCATED AT 250 WORDS)
通过不同途径(静脉注射、口服、十二指肠内给药),以0.05 - 10 mg·kg⁻¹的剂量范围,对大鼠、狗、猴和猪单次给予¹⁴C标记的(±)3 - 异丁基 - 5 - 甲基 - 1,4 - 二氢 - 2,6 - 二甲基 - 4 - (2 - 硝基苯基) - 吡啶 - 3,5 - 二羧酸酯(尼索地平,Bay k 5552)后,研究了其吸收、分布和排泄情况。[¹⁴C]尼索地平吸收迅速且几乎完全。口服给药后,大鼠血浆放射性浓度在0.9小时达到峰值,狗在1.4小时,猴在3.6小时,三种物种的标准化最大浓度处于相同范围(0.49 - 0.79)。在长达3天的观察期内,血浆放射性以42小时至54小时的半衰期消除。口服给药后,未变化的[¹⁴C]尼索地平对血浆总放射性浓度的贡献较低(峰值时,猴为0.5%,狗为3.4%),表明该化合物存在广泛的首过消除。大鼠的生物利用度估计为3.4%,狗为11.7%。[¹⁴C]尼索地平与血浆蛋白高度结合,游离分数为0.9% - 2.9%。在所有物种中,口服和静脉注射[¹⁴C]尼索地平后,放射性通过尿液和粪便/胆汁排泄迅速,且在48小时内几乎完全排出。在大鼠和狗的实验结束时,体内回收的残留量非常少(小于剂量的1.6%)。大鼠、狗和猪中,排泄的首选途径是胆汁/粪便途径,而在猴中,76%的剂量通过肾脏排泄。(摘要截取自250字)
