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在丹麦生活的越南人中,氯胍代谢由美芬妥英氧化多态性决定。

Proguanil metabolism is determined by the mephenytoin oxidation polymorphism in Vietnamese living in Denmark.

作者信息

Brøsen K, Skjelbo E, Flachs H

机构信息

Department of Clinical Pharmacology, Odense University, Denmark.

出版信息

Br J Clin Pharmacol. 1993 Aug;36(2):105-8. doi: 10.1111/j.1365-2125.1993.tb04204.x.

Abstract
  1. A sparteine/mephenytoin phenotyping test was carried out in 37 Vietnamese living in Denmark. By visual inspection the urinary S/R-mephenytoin ratio appeared to show a bimodal frequency distribution. Eight putative poor metabolizers of mephenytoin, PMm (22%), had S/R-mephenytoin ratios from 0.79 to 1.12 and 29 putative extensive metabolizers of mephenytoin, EMm, had S/R-mephenytoin ratios < or = 0.55. All of the subjects were extensive metabolizers of sparteine with urinary metabolic ratios from 0.15 to 2.4. 2. The metabolism of the antimalarial prodrug proguanil was studied in 34 of the subjects after a single oral dose of 100 mg. The median 12 h urinary recoveries of the active metabolite cycloguanil and the minor metabolite 4-chlorphenylbiguanide were 5.8 and 1.9% of the dose, respectively, in 26 EMm compared with 1.6 and 0.4%, respectively, in 8 PMm (P < 0.001, Mann-Whitney U-test). 3. There was no statistically significant correlation (Spearmans rs) between any index of proguanil metabolism and the sparteine metabolic ratio.
摘要
  1. 对37名居住在丹麦的越南人进行了司巴丁/美芬妥英表型测试。通过目视检查,尿中S/R - 美芬妥英比值似乎呈现双峰频率分布。8名推定的美芬妥英慢代谢者(PMm,22%)的S/R - 美芬妥英比值为0.79至1.12,29名推定的美芬妥英快代谢者(EMm)的S/R - 美芬妥英比值≤0.55。所有受试者都是司巴丁的快代谢者,尿代谢比值为0.15至2.4。2. 在34名受试者单次口服100 mg后,研究了抗疟前药氯胍的代谢情况。在26名快代谢者中,活性代谢物环氯胍和次要代谢物4 - 氯苯基双胍的12小时尿中回收率中位数分别为剂量的5.8%和1.9%,而在8名慢代谢者中分别为1.6%和0.4%(P < 0.001,曼 - 惠特尼U检验)。3. 氯胍代谢的任何指标与司巴丁代谢比值之间均无统计学显著相关性(斯皮尔曼rs)。

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