McNeil J J, Mihaly G W, Anderson A, Marshall A W, Smallwood R A, Louis W J
Br J Clin Pharmacol. 1981 Sep;12(3):411-5. doi: 10.1111/j.1365-2125.1981.tb01236.x.
1 Ranitidine pharmacokinetics were studied in six healthy volunteers. Following an overnight fast, doses of 20 mg intravenously 20, 40 and 100 mg orally and 100 mg orally with a standard meal, were administered to each subject on separate occasions. 2 Following intravenous administration there was a bioexponential decline in plasma levels from 576 +/- 56 ng/ml at 4 min to 10 +/- 2 ng/ml at 8 h. The distribution half-life (T 1/2 alpha) was 6.1 +/- 0.9 min, elimination half-life (T 1/2 beta) was 1.9 +/- 0.1 h, the volume of distribution (Vd beta) was 115 +/- 7 l and systemic plasma clearance (Cltp) was 709 +/- 62 ml/min. 3 Following 20 mg oral doses, peak levels were reached at 1.6 +/- 0.2 h and the systemic availability was 88 +/- 10%. Elimination half-life (T 1/2 beta) was unaffected by dose and the area under the curve increased linearly with dose and was unaffected by food. 4 Renal excretion (24 h) of unmetabolized ranitidine accounted for 50-70% of the dose with a further 1-3% appearing as desmethyl ranitidine.
1 在6名健康志愿者身上研究了雷尼替丁的药代动力学。经过一夜禁食后,分别在不同时间给每位受试者静脉注射20毫克、口服20毫克、40毫克和100毫克以及口服100毫克并搭配标准餐。
2 静脉给药后,血浆水平呈生物指数下降,从4分钟时的576±56纳克/毫升降至8小时时的10±2纳克/毫升。分布半衰期(T 1/2α)为6.1±0.9分钟,消除半衰期(T 1/2β)为1.9±0.1小时,分布容积(Vdβ)为115±7升,全身血浆清除率(Cltp)为709±62毫升/分钟。
3 口服20毫克剂量后,在1.6±0.2小时达到峰值水平,全身可用性为88±10%。消除半衰期(T 1/2β)不受剂量影响,曲线下面积随剂量呈线性增加且不受食物影响。
4 未代谢的雷尼替丁的肾排泄(24小时)占剂量的50 - 70%,另有1 - 3%以去甲基雷尼替丁的形式出现。