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Pharmacokinetics of Melamine and Cyanuric Acid and Their Combinations in F344 Rats

机译:三聚氰胺和三聚氰酸及其组合在F344大鼠中的药代动力学

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摘要

The intentional adulteration of pet food with melamine and cyanuric acid has been implicated in the kidney failure and death of a large number of cats and dogs in the United States. Although individually these compounds present low toxicity in a range of experimental animals, coexposure can lead to the formation of melamine cyanurate crystals in the nephrons and eventual kidney failure. Given this mode of action, a good understanding of the pharmacokinetic profiles of melamine and cyanuric acid and their combinations is essential to define properly the risk associated with different exposure scenarios. Previous studies have investigated the individual pharmacokinetic profiles of melamine and cyanuric acid. In this work, we report a comparison between the pharmacokinetic profiles of melamine and cyanuric acid administered individually, administered simultaneously as the individual compounds, and administered as a preformed melamine cyanurate complex. Although the oral coadministration of 1 mg/kg body weight of melamine and cyanuric acid did not alter significantly the pharmacokinetic profiles in relation to those determined upon individual oral administration of each compound, the administration of equal amounts of each triazine as the preformed melamine cyanurate complex significantly altered the pharmacokinetics, with reduced bioavailability of both compounds, lower observed maximum serum concentrations, delayed peak concentrations, and prolonged elimination half lives. These results indicate that in order to estimate properly the combined nephrotoxic potential of melamine and cyanuric acid, the experimental design of toxicological experiments and the evaluation of animal or human exposure scenarios should consider the detailed mode of exposure, with particular emphasis on any possible ex vivo formation of melamine cyanurate.
机译:在美国,三聚氰胺和氰尿酸对宠物食品的故意掺假与肾脏衰竭和大量猫和狗的死亡有关。尽管这些化合物单独在一系列实验动物中表现出低毒性,但同时暴露可能导致肾中三聚氰胺氰尿酸酯晶体的形成,并最终导致肾衰竭。在这种作用方式下,对三聚氰胺和氰尿酸及其组合的药代动力学特征有一个很好的了解对于正确定义与不同暴露场景相关的风险至关重要。先前的研究已经调查了三聚氰胺和氰尿酸的个别药代动力学特征。在这项工作中,我们报告了三聚氰胺和氰尿酸分别单独给药,作为单独化合物同时给药和作为预制三聚氰胺氰尿酸酯复合物给药时药代动力学概况之间的比较。尽管口服1 mg / kg体重的三聚氰胺和氰尿酸共同给药相对于单独口服每种化合物确定的药代动力学特征没有显着改变,但以预先形成的三聚氰胺三聚氰胺氰尿酸酯复合物的等量每种三嗪的给药方式显着改变了药代动力学,降低了两种化合物的生物利用度,降低了观察到的最大血清浓度,延迟了峰值浓度,并延长了消除半衰期。这些结果表明,为了正确估计三聚氰胺和氰尿酸的组合肾毒性潜力,毒理学实验的实验设计和动物或人类接触场景的评估应考虑详细的接触方式,尤其要强调任何可能的离体接触形成三聚氰胺氰尿酸酯。

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