头孢门铎在血液透析患者中的药代动力学。

J A Campillo, J M Lanao, A Dominguez-Gil, J M Tabernero, F Rubio
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引用次数: 0

摘要

研究了17例终末期肾功能损害患者头孢门多的药代动力学,其中10例正在进行血液透析,7例处于透析间隙期。一个开放的双室动力学模型被用来描述头孢门铎血浆浓度的双相下降,从而建立了抗生素在外周和中央室的数量以及消除的数量。所有患者均静脉注射15mg /kg体重。在血液透析期间,头孢门多的药代动力学参数为:alpha = 5.006 hr-1 beta = 0.182 hr-1 K12 = 2.598 hr-1 K21 = 2.147 hr-1 K13 = 0.441 hr-1 Vc = 5.700 l Vp = 6.190 l Vdss = 11.94 l与透析期间相比,总消除常数有所降低。多剂量的给药方案是建立在抗生素的药代动力学参数的函数终末期肾损害患者进行定期血液透析。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Pharmacokinetics of cefamandole in patients undergoing hemodialysis.

The pharmacokinetics of Cefamandole was studied in 17 patients with terminal renal impairment, 10 of which were undergoing sessions of hemodialysis while 7 were in the period between dialysis sessions. An open two-compartment kinetic model was used to describe the bi-phasic decrease of the plasma concentrations of Cefamandole thus establishing the amounts of the antibiotic in the peripheral and central compartments together with the amount eliminated. All patients received an i.v. bolus injections of 15 mg/kg body weight. During the hemodialysis sessions, the pharmacokinetic parameters of Cefamandole were the following: alpha = 5.006 hr-1 beta = 0.182 hr-1 K12 = 2.598 hr-1 K21 = 2.147 hr-1 K13 = 0.441 hr-1 Vc = 5.700 l Vp = 6.190 l Vdss = 11.94 l It may be seen that there is a decrease in the overall elimination constant compared with that obtained during the periods between the dialysis sessions. A dosage regimen of multiple doses is established as a function of the pharmacokinetic parameters of the antibiotic for patients with terminal renal impairment undergoing periodic sessions of hemodialysis.

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