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首页> 外文期刊>Journal of Medicinal Chemistry >Structure-Brain Exposure Relationships in Rat and Human Using a Novel Data Set of Unbound Drug Concentrations in Brain Interstitial and Cerebrospinal Fluids
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Structure-Brain Exposure Relationships in Rat and Human Using a Novel Data Set of Unbound Drug Concentrations in Brain Interstitial and Cerebrospinal Fluids

机译:使用脑间质和脑脊液中未结合药物浓度的新数据集,在大鼠和人类中的结构-脑暴露关系

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摘要

New experimental methodologies were applied to measure the unbound brain-to-plasma concentration ratio (K-p,K-uu,K-brain) and the unbound CSF-to-plasma concentration ratio (K-p,K-uu,K-CSF) in rats for 43 structurally diverse drugs. The relationship between chemical structure and K-p,K-uu,K-brain was dominated by hydrogen bonding. Contrary to popular understanding based on the total brain-to-plasma concentration ratio (logBB), lipophilicity was not a determinant of unbound brain exposure. Although changing the number of hydrogen bond acceptors is a useful design strategy for optimizing K-p,K-uu,K-brain, future improvement of in silico prediction models is dependent on the accommodation of active drug transport. The structure-brain exposure relationships found in the rat also hold for humans, since the rank order of the drugs was similar for human and rat K-p,K-uu,K-CSF. This cross-species comparison was supported by K-p,K-uu,K-CSF being within 3-fold of K-p,K-uu,K-brain in the rat for 33 of 39 drugs. It was, however, also observed that K-p,K-uu,K-CSF overpredicts K-p,K-uu,K-brain for highly effluxed drugs, indicating lower efflux capacity of the blood-cerebrospinal fluid barrier compared to the blood-brain barrier.
机译:应用新的实验方法来测量大鼠的未结合脑与血浆的浓度比(Kp,K-uu,K-brain)和未结合脑脊液与血浆的浓度比(Kp,K-uu,K-CSF)用于43种结构多样的药物。化学结构与K-p,K-uu,K-脑之间的关系主要由氢键决定。与基于总脑血浆浓度比(logBB)的流行理解相反,亲脂性不是决定未受束缚的大脑暴露的因素。尽管更改氢键受体的数量是优化K-p,K-uu,K-脑的有用设计策略,但是计算机模拟模型的未来改进取决于活性药物转运的适应性。在大鼠中发现的结构脑暴露关系也适用于人类,因为药物的排名顺序与人和大鼠的K-p,K-uu,K-CSF相似。 39种药物中的33种在大鼠中K-p,K-uu,K-CSF在K-p,K-uu,K-脑的3倍以内,这一跨物种比较得到了支持。但是,还观察到Kp,K-uu,K-CSF对高排量药物高估了Kp,K-uu,K-脑,这表明血脑脊髓液屏障的流出能力比血脑屏障低。

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