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血脑屏障的通透性:药物及生理重要化合物的转运分子机制

Permeability of the Blood-Brain Barrier: Molecular Mechanism of Transport of Drugs and Physiologically Important Compounds.

作者信息

Fong Clifford W

机构信息

Eigenenergy, Adelaide, SA, Australia,

出版信息

J Membr Biol. 2015 Aug;248(4):651-69. doi: 10.1007/s00232-015-9778-9. Epub 2015 Feb 13.

Abstract

A new molecular model for the permeability of drugs and other physiologically important compounds to cross the blood-brain barrier has been developed. Permeability (log PS) is dependant on desolvation, lipophilicity, molecular volume and dipole moment. Previous models for BBB permeability have not considered desolvation and dipole moment as critical factors. The model applies to passive diffusion processes, and some facilitated diffusion processes. Passive permeability models may not apply to active transport processes, where complex membrane protein binding processes (e.g. stereoselectivity) are involved. Model phosphatidylcholine lipid bilayer membranes have been used to evaluate how charged or polar neutral compounds can interact through their molecular dipoles with the cell membrane to induce electromechanical changes in the cell membrane which facilitate permeation. The free energy of solvation in n-octanol has been shown to be a good measure of membrane lipophilicity by calculating the solvation free energy of a model PC lipid membrane in a series of closely related alcohols. The passive diffusion model for alcohols correlates with the known modulation of membrane bilayers which showed a size-dependent "cut-off" point in potency. For most drugs and related molecules, the neutral species are the permeating species.

摘要

一种用于药物及其他生理重要化合物穿越血脑屏障通透性的新分子模型已被开发出来。通透性(log PS)取决于去溶剂化、亲脂性、分子体积和偶极矩。先前的血脑屏障通透性模型并未将去溶剂化和偶极矩视为关键因素。该模型适用于被动扩散过程以及一些易化扩散过程。被动通透性模型可能不适用于涉及复杂膜蛋白结合过程(如立体选择性)的主动转运过程。已使用模型磷脂酰胆碱脂质双层膜来评估带电或极性中性化合物如何通过其分子偶极与细胞膜相互作用,从而在细胞膜中诱导机电变化以促进渗透。通过计算一系列密切相关醇类中模型PC脂质膜的溶剂化自由能,已表明正辛醇中的溶剂化自由能是膜亲脂性的良好度量。醇类的被动扩散模型与已知的膜双层调节相关,该调节在效力上显示出大小依赖性的“截止”点。对于大多数药物和相关分子,中性物种是渗透物种。

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