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Drug design tools--in silico, in vitro and in vivo ADME/PK prediction and interpretation: is PK in monkey an essential part of a good human PK prediction?

机译:药物设计工具-计算机模拟,体外和体内ADME / PK预测和解释:猴子的PK是否是人类良好PK预测的重要组成部分?

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摘要

Quantitative human pharmacokinetic (PK) predictions play a critical role in assessing the quality of potential drug candidates and in selecting a human starting dose for clinical evaluation, where the parameters of clearance, volume of distribution, and bioavailability as well as the plasma concentration time profiles are the desired endpoints. While there are numerous reports validating the use of different methods for predictions, it still remains an open question as to what animal species to include when extrapolating the animal PK to human. Given toxicological assessment is generally conducted in two species, a rodent and a non-rodent species, prior to evaluation in human subjects, rat, dog and/or monkey are typically the species ADME scientists employ to evaluate PK. However, the question is, can we achieve an adequate prediction without the use of larger species such as monkey? In the end, the data and tools utilized for human PK predictions will depend on a number of factors such as information from observed human PK for structurally related compounds; the primary mechanism of clearance, and the availability of in silico and in vitro tools applicable to the respective clearance mechanism. Despite these dependencies, for most situations, adequate predictions can be achieved without the use of monkey PK for predicting human.
机译:定量人类药代动力学(PK)预测在评估潜在药物候选者的质量以及选择用于临床评估的人类起始剂量方面起着关键作用,其中清除率,分布体积和生物利用度以及血浆浓度时间分布参数是所需的端点。尽管有许多报道证实使用不同的方法进行预测,但是当将动物PK推算给人类时,仍然包括一个尚待解决的问题。给定毒理学评估一般是在啮齿动物和非啮齿动物两个物种中进行的,然后在人类受试者中进行评估,老鼠,狗和/或猴子通常是ADME科学家用来评估PK的物种。但是,问题是,在不使用猴子等较大物种的情况下,我们能否实现足够的预测?最后,用于人类PK预测的数据和工具将取决于许多因素,例如来自观察到的人类PK的结构相关化合物的信息;清除的主要机制,以及适用于各个清除机制的计算机和体外工具的可用性。尽管存在这些依赖性,但在大多数情况下,无需使用猴子PK来预测人类就可以实现足够的预测。

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