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体外跨膜单层通透性计算:常被遗忘的假设

In vitro trans-monolayer permeability calculations: often forgotten assumptions.

作者信息

Youdim Kuresh A, Avdeef Alex, Abbott N Joan

机构信息

Antioxidant Research Group Wolfson Centre for Age-Related Diseases Guy's, King's and St Thomas' School of Biomedical Sciences King's College, London, SE1 1UL, UK.

出版信息

Drug Discov Today. 2003 Nov 1;8(21):997-1003. doi: 10.1016/s1359-6446(03)02873-3.

Abstract

In designing effective therapeutic strategies, novel drugs must exhibit favorable pharmacokinetic properties. The physicochemical characteristics of a drug, such as pK(a), molecular weight, solubility and lipophilicity, will influence the way the drug partitions from the aqueous phase into membranes, and thus, will influence its ability to cross cellular barriers, such as the lining of the gastrointestinal tract and the blood-brain barrier. Physicochemical characteristics also influence the degree to which a drug is able to cross a barrier layer, and the route by which it does this; whether transcellular (across the cells)-by diffusion, carrier-mediated transport or transcytosis-or paracellular-by diffusing through the tight junctions between the cells. The in vitro model systems that are currently employed to screen the permeation characteristics of a drug often represent a compromise between high throughput with low predictive potential and low throughput with high predictive potential. Here, we will examine the way in which in vitro cellular permeability assays are often performed and the assumptions that are implied but sometimes forgotten, and we will make simple suggestions for improving the methodological techniques and mathematical equations used to determine drug permeability.

摘要

在设计有效的治疗策略时,新型药物必须具备良好的药代动力学特性。药物的物理化学特性,如pK(a)、分子量、溶解度和亲脂性,会影响药物从水相分配到膜中的方式,进而影响其穿越细胞屏障(如胃肠道内衬和血脑屏障)的能力。物理化学特性还会影响药物穿越屏障层的程度及其穿越途径;是通过跨细胞(穿过细胞)——通过扩散、载体介导的转运或转胞吞作用——还是通过细胞旁——通过细胞间紧密连接扩散。目前用于筛选药物渗透特性的体外模型系统往往是高通量但预测潜力低与低通量但预测潜力高之间的折中。在此,我们将研究体外细胞通透性测定通常的进行方式以及隐含但有时被遗忘的假设,并对用于确定药物通透性的方法技术和数学方程的改进提出简单建议。

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