伯氨喹在人体中的药代动力学。I. 绝对生物利用度及剂量大小影响的研究。
Pharmacokinetics of primaquine in man. I. Studies of the absolute bioavailability and effects of dose size.
作者信息
Mihaly G W, Ward S A, Edwards G, Nicholl D D, Orme M L, Breckenridge A M
出版信息
Br J Clin Pharmacol. 1985 Jun;19(6):745-50. doi: 10.1111/j.1365-2125.1985.tb02709.x.
The pharmacokinetics of primaquine have been examined in five healthy volunteers who received single oral doses of 15, 30 and 45 mg of the drug, on separate occasions. Each subject received an i.v. tracer dose of [14C]-primaquine (7.5 microCi), simultaneously with the 45 mg oral dose. Absorption of primaquine was virtually complete with a mean absolute bioavailability of 0.96 +/- 0.08. Elimination half-life, oral clearance and apparent volume of distribution for both primaquine and the carboxylic acid metabolite were unaffected by either dose size, or route of administration. The relationships between area under the curve and dose size were linear for both primaquine (r = 0.99, P less than or equal to 0.01) and its carboxylic acid metabolite (r = 0.99, p less than or equal to 0.01). The mean whole blood to plasma concentration ratios were determined for primaquine (0.81), and for the carboxylic acid metabolite of primaquine (0.84). Primaquine is a low clearance compound (CL = 24.2 +/- 7.4 l h-1), is extensively distributed into body tissues (V = 242.9 +/- 69.5 l) and is not subject to extensive first pass metabolism.
已在5名健康志愿者身上研究了伯氨喹的药代动力学,这些志愿者在不同时间分别接受了15毫克、30毫克和45毫克的单次口服剂量。每名受试者在接受45毫克口服剂量的同时,静脉注射了示踪剂量的[14C] - 伯氨喹(7.5微居里)。伯氨喹的吸收几乎完全,平均绝对生物利用度为0.96±0.08。伯氨喹及其羧酸代谢物的消除半衰期、口服清除率和表观分布容积均不受剂量大小或给药途径的影响。伯氨喹(r = 0.99,P≤0.01)及其羧酸代谢物(r = 0.99,p≤0.01)的曲线下面积与剂量大小之间的关系均呈线性。测定了伯氨喹(0.81)及其羧酸代谢物(0.84)的平均全血与血浆浓度比。伯氨喹是一种低清除率化合物(CL = 24.2±7.4升/小时),广泛分布于身体组织中(V = 242.9±69.5升),且不存在广泛的首过代谢。
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