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Drug structure–transport relationships

机译:药物结构与运输的关系

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Malcolm Rowland has greatly facilitated an understanding of drug structure–pharmacokinetic relationships using a physiological perspective. His view points, covering a wide range of activities, have impacted on my own work and on my appreciation and understanding of our science. This overview summarises some of our parallel activities, beginning with Malcolm’s work on the pH control of amphetamine excretion, his work on the disposition of aspirin and on the application of clearance concepts in describing the disposition of lidocaine. Malcolm also spent a considerable amount of time developing principles that define solute structure and transport/pharmacokinetic relationships using in situ organ studies, which he then extended to involve the whole body. Together, we developed a physiological approach to studying hepatic clearance, introducing the convection–dispersion model in which there was a spread in blood transit times through the liver accompanied by permeation into hepatocytes and removal by metabolism or excretion into the bile. With a range of colleagues, we then further developed the model and applied it to various organs in the body. One of Malcolm’s special interests was in being able to apply this knowledge, together with an understanding of physiological differences in scaling up pharmacokinetics from animals to man. The description of his many other activities, such as the development of clearance concepts, application of pharmacokinetics to the clinical situation and using pharmacokinetics to develop new compounds and delivery systems, has been left to others.
机译:马尔科姆·罗兰德(Malcolm Rowland)使用生理观点极大地促进了对药物结构与药代动力学关系的理解。他的观点涵盖了广泛的活动,对我自己的工作以及对科学的欣赏和理解产生了影响。概述概述了我们的一些并行活动,从马尔科姆(Malcolm)在控制苯丙胺排泄的pH值方面的工作,他在阿司匹林的处置以及清除概念在描述利多卡因处置方面的应用开始。马尔科姆(Malcolm)还花费大量时间使用原位器官研究来开发定义溶质结构和转运/药代动力学关系的原理,然后他将其扩展到涉及整个身体。我们共同开发了一种研究肝清除率的生理方法,引入了对流扩散模型,其中血液在肝脏中的传播时间有所扩散,并伴随着渗透进入肝细胞,并通过代谢或排泄进入胆汁而被清除。然后,我们与许多同事一起进一步开发了该模型,并将其应用于体内的各个器官。马尔科姆(Malcolm)的特殊兴趣之一是能够运用这些知识,以及对从动物到人的药代动力学按比例放大的生理差异的理解。他的许多其他活动的描述,例如清除概念的开发,将药代动力学应用于临床情况以及使用药代动力学来开发新化合物和递送系统,都留给了其他人。

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