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氨苯砜及乙酰化氨苯砜在血清和唾液中的药代动力学。

The pharmacokinetics of dapsone and acetylated dapsone in serum and saliva.

作者信息

Lammintausta K, Kangas L, Lammintausta R

出版信息

Int J Clin Pharmacol Biopharm. 1979 Apr;17(4):159-63.

PMID:447435
Abstract

The concentrations of dapsone (DDS) and its acetylated derivatives (MADDS and DADDS) were determined in the serum and saliva after one oral dose of dapsone until 72 hr. The peak serum concentrations of DDS and MADDS were reached, on average, at 3.8--4.3 hr after the dosage. The amounts of DADDS were negligible. The elimination half-life of the first order kinetics was, on average, at 20--21 hr for both DDS and MADDS. The study group included 6 rapid acetylators and 4 slow acetylators with the mean ratios MADDS/DDS 1.0 and 0.19, respectively. No difference in the pharmacokinetics of DDS or MADDS could be seen between the rapid and slow acetylators. The protein-free fractions of DDS and MADDS were 50 and 41 per cent, respectively, of the total serum concentrations as measured at 8 and 32 hr after the dosage. The salivary concentration of DDS was, on average, 49 per cent of the total serum concentration during the whole study period. The salivary concentration of MADDS was 40 per cent, respectively. The elimination half-life of DDS and MADDS in saliva did not differ from that in serum. Between the salivary and serum protein-free concentrations a strict correlation existed (p less than 0.001). The salivary concentration of dapsone and its monoacetyl derivative reflect the protein-free, active drug in serum.

摘要

单次口服氨苯砜后72小时内,对血清和唾液中氨苯砜(DDS)及其乙酰化衍生物(MADDS和DADDS)的浓度进行了测定。给药后,DDS和MADDS的血清峰值浓度平均在3.8 - 4.3小时达到。DADDS的量可忽略不计。DDS和MADDS的一级动力学消除半衰期平均为20 - 21小时。研究组包括6名快速乙酰化者和4名慢速乙酰化者,MADDS/DDS的平均比值分别为1.0和0.19。快速和慢速乙酰化者之间在DDS或MADDS的药代动力学方面未见差异。给药后8小时和32小时测得的DDS和MADDS的游离蛋白部分分别占血清总浓度的50%和41%。在整个研究期间,DDS的唾液浓度平均为血清总浓度的49%。MADDS的唾液浓度分别为40%。DDS和MADDS在唾液中的消除半衰期与血清中的无差异。唾液和血清游离蛋白浓度之间存在严格的相关性(p小于0.001)。氨苯砜及其单乙酰衍生物的唾液浓度反映了血清中游离蛋白的活性药物。

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