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口服脂质体递药系统靶向脑部给药是否可行?

Is oral lipid-based delivery for drug targeting to the brain feasible?

机构信息

School of Pharmacy, University of Nottingham, Nottingham, Nottinghamshire NG7 2RD, UK.

Division of Food, Nutrition and Dietetics, University of Nottingham, Sutton Bonington Campus, Loughborough, Leicestershire LE12 5RD, UK.

出版信息

Eur J Pharm Biopharm. 2022 Mar;172:112-122. doi: 10.1016/j.ejpb.2022.02.004. Epub 2022 Feb 8.

Abstract

This review outlines the feasibility of oral lipid-based targeted delivery of drugs to the brain, including permeation of the central nervous system's (CNS) protective blood-brain barrier (BBB). The structure of the BBB and disruption caused by varying disease states highlights the need for disease-specific approaches to alter permeation. Disruption during disease state, and the effects of certain molecules on the barrier, demonstrate the possibility of exploiting such BBB disruption for drug delivery. Many administration methods can be used to target the brain, but oral administration is considered ideal for chronic, long-term illnesses. Several lipids that have been shown to facilitate drug delivery into the brain after systemic administration, but could also be delivered orally, are discussed, including oleic acid, triolein, alkylglycerol, and conjugates of linoleic and myristic acids. Current data reveal the potential for the use of such lipids as part of oral formulations for delivery to the brain by reaching sufficient plasma levels after administration to increase the permeability of the BBB. However, gaps in the literature remain regarding the concentrations and form of most lipids required to produce the desired effects. The use of lipids via oral delivery for brain targeting has not been investigated thoroughly enough to determine with certainty if similar permeability-enhancing effects would be observed as for parenteral administration. In conclusion, further research to fill research gaps is needed, but the limited evidence suggests that oral lipid-based drug delivery for brain targeting is potentially feasible.

摘要

本文概述了将药物经口服递送至脑内的靶向脂质传递的可行性,包括穿透中枢神经系统(CNS)的保护性血脑屏障(BBB)。BBB 的结构以及各种疾病状态引起的破坏突出表明需要针对特定疾病的方法来改变通透性。疾病状态下的破坏以及某些分子对屏障的影响表明,利用这种 BBB 破坏进行药物递送是有可能的。有许多给药方法可用于靶向脑部,但口服给药被认为是治疗慢性、长期疾病的理想选择。本文讨论了几种已经显示出在全身给药后能够促进药物递送至脑部,但也可以口服给药的脂质,包括油酸、三油酸甘油酯、烷基甘油以及亚油酸和肉豆蔻酸的轭合物。目前的数据显示,这些脂质有可能作为口服制剂的一部分,通过在给药后达到足够的血浆水平来增加 BBB 的通透性,从而实现向脑部的递送。然而,关于大多数脂质达到所需效果所需的浓度和形式,文献中仍存在空白。通过口服途径使用脂质进行脑靶向的研究还不够充分,无法确定是否会观察到与肠外给药类似的通透性增强效果。总之,需要进一步研究以填补研究空白,但有限的证据表明,口服基于脂质的药物传递用于脑靶向是具有潜力的。

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