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首页> 外文期刊>Expert opinion on drug discovery >Mechanistic models enable the rational use of in vitro drug-target binding kinetics for better drug effects in patients
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Mechanistic models enable the rational use of in vitro drug-target binding kinetics for better drug effects in patients

机译:机理模型可以合理利用体外药物-靶标结合动力学,为患者带来更好的药物作用

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摘要

Introduction: Drug-target binding kinetics are major determinants of the time course of drug action for several drugs, as clearly described for the irreversible binders omeprazole and aspirin. This supports the increasing interest to incorporate newly developed high-throughput assays for drug-target binding kinetics in drug discovery. A meaningful application of in vitro drug-target binding kinetics in drug discovery requires insight into the relation between in vivo drug effect and in vitro measured drug-target binding kinetics.Areas covered: In this review, the authors discuss both the relation between in vitro and in vivo measured binding kinetics and the relation between in vivo binding kinetics, target occupancy and effect profiles.Expert opinion: More scientific evidence is required for the rational selection and development of drug-candidates on the basis of in vitro estimates of drug-target binding kinetics. To elucidate the value of in vitro binding kinetics measurements, it is necessary to obtain information on system-specific properties which influence the kinetics of target occupancy and drug effect. Mathematical integration of this information enables the identification of drug-specific properties which lead to optimal target occupancy and drug effect in patients.
机译:简介:药物-靶标的结合动力学是几种药物在药物作用过程中的主要决定因素,如不可逆粘合剂奥美拉唑和阿司匹林已明确描述。这支持了越来越多的兴趣将新开发的高通量分析方法用于药物发现中的药物靶标结合动力学。体外药物-靶标结合动力学在药物发现中的有意义的应用需要洞悉体内药物作用与体外测量的药物-靶标结合动力学之间的关系。涵盖的领域:在这篇综述中,作者讨论了体外与药物之间的关系专家意见:基于体外药物靶点估计值,合理选择和开发候选药物还需要更多的科学证据结合动力学。为了阐明体外结合动力学测量的价值,有必要获得有关系统特异性特性的信息,这些信息会影响靶标占有率和药物作用的动力学。通过对这些信息进行数学整合,可以识别药物特有的特性,从而使患者达到最佳的靶标占有率和药物作用。

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