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Effects of pharmaceuticals and other active chemicals at biological targets: mechanisms, interactions, and integration into PB-PK/PD models.

机译:药物和其他活性化学品对生物学目标的影响:机理,相互作用和整合到PB-PK / PD模型中。

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摘要

Biologically active molecules, that is pharmaceuticals and other chemical substances, exert their therapeutic and/or toxic effects by complex interactions with their biological targets/active sites. This review discusses the factors and processes governing the kinetics and effects of active molecules at their cellular targets, the chain of events leading to clinical effects, and the crosstalk between regulatory pathways controlling these processes. Special attention is given to the discussion of effects of a single drug or other chemical on multiple targets, to the interaction of multiple ligands with a single target/receptor and the effects of single ligand-target complexes on multiple signal transduction pathways, and to the control of physiological functions, such as regulation of blood glucose levels, by numerous primary mechanisms acting on different cellular targets. Physiologically based-pharmacokinetic/pharmacodynamic (PB-PK/PD) models are of great value for the design of active principles by the pharmaceutical industry and for the optimization and individualization of patient therapy. Experimental results from in vitro and in vivo studies can be used for building such models. On the other hand, properly designed models and simulation can contribute to a better design of experiments. Much of what is presented in this article applies equally well to drugs and other chemicals. Unless specified otherwise, reference to drugs applies also to other chemicals. This review is based on an expert meeting organized by COST Action B25 held in Eilat, Israel, on 14 - 15 February 2008. The authors have prepared this article to reflect the presentations and discussions at that meeting.
机译:生物活性分子,即药物和其他化学物质,通过与其生物靶标/活性位点的复杂相互作用而发挥其治疗和/或毒性作用。这篇综述讨论了控制活性分子在其细胞靶标上的动力学和作用的因素和过程,导致临床影响的事件链以及控制这些过程的调节途径之间的串扰。特别注意单个药物或其他化学物质对多个靶标的影响,多个配体与单个靶标/受体之间的相互作用以及单个配体-靶标复合物对多个信号转导途径的影响,以及通过作用于不同细胞靶标的许多主要机制来控制生理功能(例如调节血糖水平)。基于生理学的药代动力学/药效学(PB-PK / PD)模型对于制药行业设计有效成分以及优化和个性化患者治疗具有重要价值。体外和体内研究的实验结果可用于建立此类模型。另一方面,正确设计的模型和仿真可以有助于更好地设计实验。本文介绍的大部分内容同样适用于药物和其他化学药品。除非另有说明,否则对药物的引用也适用于其他化学品。这篇评论是基于COST Action B25在2008年2月14日至15日在以色列埃拉特举行的专家会议的基础上进行的。作者准备了本文,以反映该次会议上的介绍和讨论。

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