十二烷二酸在大鼠体内的药动学

A. Bertuzzi, A. De Gaetano, A. Gandolfi, A. Greco, G. Mingrone, S. Salinari
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引用次数: 1

摘要

使用中链二羧酸,壬二酸和癸二酸,作为总肠外营养的能量底物W M最近提出[1,2],因为这些酸可能比长链和中链甘油三酯具有代谢优势。然而,大量给药剂量的壬二酸和己二酸通过尿液排出,因此,就能量产量而言,这些酸在肠外营养中的适用性似乎值得怀疑[3,4]。十二烷二酸(C12)在大鼠中获得了令人鼓舞的结果,其尿排泄量非常低151。在本文中,我们通过一个具有饱和组织摄取的药代动力学模型来分析(5)中的数据,使用了一种考虑到ode1 / 9 / 3的个体间差异的估计方法。
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 dodecanedioic acid in rat
The use of medium-chain dicarboxylic acjds, azelaic and sebacic acid, as energy substrates in total parenteral nutrition W M recently proposed [ 1 ,2\ , since these acids may have metabolic advantages over long-chain and medium-chain triglycerides. However, a large amount of the administered dose of azelaic and sebacic acid is excreted in the urine, so that the suitability of these acids in parenteral nutrition appears to be doubtful in terms of energetic yield [3,4]. Encouraging results were obtained in rat with the dodecanedioic acid (C12), which presents very low urinary excretion 151. In this paper we analyze the data in ( 5 ) by inems of a pharmacokinetic model with saturable tissue uptake, using an estimation method that tnkes into account the interindividual variability of in ode1 par nine t ers .
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