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乙酰化代谢表型在普鲁卡因胺药代动力学及不良反应中的意义

Significance of acetylator phenotype in pharmacokinetics and adverse effects of procainamide.

作者信息

Ylitalo P, Ruosteenoja R, Leskinen O, Metsä-Ketelä T

出版信息

Eur J Clin Pharmacol. 1983;25(6):791-5. doi: 10.1007/BF00542522.

Abstract

The pharmacokinetics and development of antinuclear antibodies (ANAs) during procainamide (PA) therapy were studied in 35 patients with ventricular arrhythmias. Sixteen of the subjects were rapid and 19 were slow acetylators. Twenty-six of them (13 rapid and 13 slow acetylators) received PA therapy (2.4g sustained-release PA X HCl daily in three doses) for at least 16 weeks. On maintenance therapy, rapid acetylators had insignificantly lower serum PA concentrations and slightly higher N-acetylprocainamide (NAPA) concentrations than slow acetylators. The unchanged PA fraction (PA/PA + NAPA) in the rapid acetylators was somewhat lower than in the slow acetylators. Rapid acetylators excreted more NAPA in urine than did slow acetylators (p less than 0.05), whereas the difference in PA excretion was not significant. More than 80% of the given drug was excreted as PA and NAPA. Spontaneous or exercise-induced arrhythmias were recorded in 6 rapid and 8 slow acetylators. ANAs (titre at least 20) appeared in 6 rapid and 8 slow acetylators. The mean time until ANA development in rapid acetylators was only marginally longer than in slow acetylators. The results suggest that acetylation phenotyping is not of great significance in predicting the development of ANAs during PA therapy.

摘要

对35例室性心律失常患者进行了普鲁卡因胺(PA)治疗期间的药代动力学及抗核抗体(ANA)产生情况的研究。其中16例为快乙酰化者,19例为慢乙酰化者。26例患者(13例快乙酰化者和13例慢乙酰化者)接受PA治疗(每日2.4g缓释PA盐酸盐,分三次服用)至少16周。在维持治疗阶段,快乙酰化者的血清PA浓度略低于慢乙酰化者,N - 乙酰普鲁卡因胺(NAPA)浓度略高于慢乙酰化者。快乙酰化者中未变化的PA比例(PA/PA + NAPA)略低于慢乙酰化者。快乙酰化者尿中排泄的NAPA比慢乙酰化者多(p < 0.05),而PA排泄的差异不显著。超过80%的给药药物以PA和NAPA形式排泄。6例快乙酰化者和8例慢乙酰化者记录到自发性或运动诱发的心律失常。6例快乙酰化者和8例慢乙酰化者出现ANA(滴度至少为20)。快乙酰化者ANA产生的平均时间仅比慢乙酰化者略长。结果表明,乙酰化表型在预测PA治疗期间ANA的产生方面意义不大。

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