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Plasma disposition of vitamin K1 in relation to anticoagulant poisoning.

机译:血浆维生素K1与抗凝剂中毒有关。

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摘要

The disposition of vitamin K1, after intravenous (10 mg) and oral doses (10 mg and 50 mg) was studied in six healthy male subjects. After intravenous administration, the plasma concentration-time profile was adequately fitted with an average terminal half-life of 1.7 h. After oral administration (10 mg and 50 mg) the availability of vitamin K showed marked inter-individual variation (10-63%). With the higher dose intra-individual variation was also observed. Experiments in brodifacoum-anticoagulated rabbits demonstrate that the duration of action of a pharmacological dose (10 mg/kg) is short (9 h) and that high plasma concentrations (ca 1 microgram/ml) of the vitamin are required to drive clotting factor synthesis during maximum coumarin anticoagulation. Taken collectively, these data indicate that the short duration of action of vitamin K, frequently observed in cases of coumarin poisoning, is a consequence of requirements for high vitamin K concentrations and rapid clearance of the vitamin.
机译:在六个健康的男性受试者中,研究了静脉内(10 mg)和口服(10 mg和50 mg)后维生素K1的处置。静脉内给药后,血浆浓度-时间曲线足以满足1.7 h的平均终末半衰期。口服(10毫克和50毫克)后,维生素K的利用率显示出明显的个体差异(10-63%)。随着剂量的增加,还观察到个体内部差异。 Brodifacoum抗凝兔的实验表明,药理作用(10 mg / kg)的作用持续时间短(9 h),需要高血浆浓度(ca 1微克/ ml)的维生素来驱动凝血因子的合成在最大香豆素抗凝期间。综上所述,这些数据表明,在香豆素中毒的情况下经常观察到维生素K的作用持续时间短,这是对维生素K高浓度和快速清除维生素的要求的结果。

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