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阿维A及其13-顺式代谢物在银屑病患者中的药代动力学。

The pharmacokinetics of acitretin and its 13-cis-metabolite in psoriatic patients.

作者信息

Larsen F G, Jakobsen P, Eriksen H, Grønhøj J, Kragballe K, Nielsen-Kudsk F

机构信息

Department of Dermatology, Marselisborg Hospital, Aarhus, Denmark.

出版信息

J Clin Pharmacol. 1991 May;31(5):477-83. doi: 10.1002/j.1552-4604.1991.tb01907.x.

Abstract

The synthetic retinoic acid derivative acitretin has recently been introduced for the treatment of severe psoriasis. Hitherto, the use of the carboxylic acid ester analogue, etretinate, has been hampered by an extremely long elimination half-life of up to 120 days for this drug. In the presented study, 12 patients with severe psoriasis were treated with 30 mg acitretin daily for a period of 6 months. The maximum plasma concentration of the drug occurred within about 0.9 to 4.6 hours with an apparent absorption half-life ranging from 0.2 to 1.7 hours and with half-lives of the distribution phase within the range of 1.2 to 3.5 hours. After stopping therapy, the terminal elimination half-life of acitretin varied between 16.5 and 111.1 hours (mean: 47.1 hr +/- 29.8 SD), whereas that for the 13-cis-metabolite varied between 36.5 and 249.4 hours (mean: 119.4 hr +/- 73.4 SD). Suction blister fluid concentrations of both the parent drug and metabolite were lower than plasma concentrations. The mean concentration of serum triglycerides was significantly elevated during the course of therapy, but still remained within the normal range. Saliva concentrations of drug and metabolite at steady-state were below 1 ng/mL. It is not possible from the observed half-lives of acitretin and its 13-cis-metabolite to draw any definite conclusion with regard to the anticonceptional period after acitretin therapy in psoriatic patients.

摘要

合成视黄酸衍生物阿维A最近已被用于治疗重度银屑病。迄今为止,羧酸酯类似物依曲替酯的使用受到该药物长达120天的极长消除半衰期的限制。在本研究中,12例重度银屑病患者每天服用30mg阿维A,持续6个月。药物的最大血浆浓度在约0.9至4.6小时内出现,表观吸收半衰期为0.2至1.7小时,分布相半衰期在1.2至3.5小时范围内。停止治疗后,阿维A的终末消除半衰期在16.5至111.1小时之间(平均:47.1小时±29.8标准差),而13 - 顺式代谢物的半衰期在36.5至249.4小时之间(平均:119.4小时±73.4标准差)。母体药物和代谢物的吸疱液浓度均低于血浆浓度。治疗过程中血清甘油三酯的平均浓度显著升高,但仍在正常范围内。稳态时药物和代谢物的唾液浓度低于1ng/mL。根据观察到的阿维A及其13 - 顺式代谢物的半衰期,无法就银屑病患者阿维A治疗后的避孕期得出任何明确结论。

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