Shibasaki M, Usui T, Inagaki O, Asano M, Takenaka T
Cardiovascular Research Laboratory, Yamanouchi Pharmaceutical Co. Ltd., Tsukuba Research Center, Ibaraki Prefecture, Japan.
J Pharm Pharmacol. 1994 Jan;46(1):68-72. doi: 10.1111/j.2042-7158.1994.tb03723.x.
The pharmacokinetics and cardiovascular effects of YM-21095 ((2RS), (3S)-3-[N alpha-[1,4-dioxo-4-morpholino-2-(1-naphthylmethyl)- butyl]-L-histidylamino]-4-cyclohexyl-1-[(1-methyl-5-tetrazolyl)thi o]-2-butanol), a potent renin inhibitor, have been studied in beagle dogs and squirrel monkeys. Plasma levels of YM-21095 after 3 mg kg-1 intravenous dosing to dogs declined biphasically and fitted a two-compartment model. Kinetics were as follows: t1/2 alpha = 4.9 +/- 0.2 min, t1/2 beta = 2.76 +/- 0.79 h, Vdss = 3.86 +/- 1.04 L kg-1, plasma clearance = 2.22 +/- 0.39 L kg-1, and AUC = 1445 +/- 266 ng h mL-1. After 30 mg kg-1 oral dose, maximum plasma concentration, tmax and AUC of YM-21095 were 28.8 +/- 9.6 ng mL-1, 0.25 h and 23.6 +/- 7.7 ng h mL-1, respectively. Systemic bioavailability as determined on the basis of the ratio of AUC after intravenous and oral dose was 0.16 +/- 0.04%. In conscious, sodium-depleted monkeys, YM-21095 at an oral dose of 30 mg kg-1 lowered systolic blood pressure and inhibited plasma renin activity without affecting heart rate and plasma aldosterone concentration. Maximum plasma concentration of YM-21095 after 30 mg kg-1 oral dose to monkeys was 71.8 +/- 41.5 ng mL-1, which was reached 0.5 h after the dose. At equihypotensive doses, captopril and nicardipine increased plasma renin activity markedly and slightly, respectively.(ABSTRACT TRUNCATED AT 250 WORDS)
强效肾素抑制剂YM-21095((2RS),(3S)-3-[Nα-[1,4-二氧代-4-吗啉代-2-(1-萘基甲基)-丁基]-L-组氨酰氨基]-4-环己基-1-[(1-甲基-5-四唑基)硫代]-2-丁醇)的药代动力学和心血管效应已在比格犬和松鼠猴身上进行了研究。给犬静脉注射3mg/kg剂量后,YM-21095的血浆浓度呈双相下降,并符合二室模型。动力学参数如下:t1/2α = 4.9±0.2分钟,t1/2β = 2.76±0.79小时,Vdss = 3.86±1.04L/kg,血浆清除率 = 2.22±0.39L/kg,AUC = 1445±266ng·h/mL-1。口服30mg/kg剂量后,YM-21095的最大血浆浓度、tmax和AUC分别为28.8±9.6ng/mL-1、0.25小时和23.6±7.7ng·h/mL-1。根据静脉注射和口服剂量后的AUC比值确定的系统生物利用度为0.16±0.04%。在清醒、缺钠的猴子中,口服30mg/kg剂量的YM-21095可降低收缩压并抑制血浆肾素活性,而不影响心率和血浆醛固酮浓度。给猴子口服30mg/kg剂量后,YM-21095的最大血浆浓度为71.8±41.5ng/mL-1,在给药后0.5小时达到。在等降压剂量下,卡托普利和尼卡地平分别显著和轻微增加血浆肾素活性。(摘要截断于250字)
