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脂质纳米制剂在治疗神经紊乱中的应用

Lipid-based nanoformulations in the treatment of neurological disorders.

机构信息

Department of Pharmacology, College of Clinical Pharmacy, Imam Abdulrahman Bin Faisal University, Dammam, Saudi Arabia.

Department of Pharmacy, School of Medical and Allied Sciences, K.R. Mangalam University, Gurgaon, India.

出版信息

Drug Metab Rev. 2020 Feb;52(1):185-204. doi: 10.1080/03602532.2020.1726942. Epub 2020 Mar 2.

DOI:10.1080/03602532.2020.1726942
PMID:32116044
Abstract

The neurological disorders affect millions of people worldwide, and are bracketed as the foremost basis of disability-adjusted life years (DALYs). The treatment options are symptomatic and often the movement of drugs is restricted by a specialized network of endothelial cell layers (adjoined by tight cell-to-cell junction proteins; occludin, claudins, and junctional adhesion molecules), pericytes and astroglial foot processes. In recent years, advances in nanomedicine have led to therapies that target central nervous system (CNS) pathobiology via altering signaling mechanisms such as activation of PI3K/Akt pathway in ischemic stroke arrests apoptosis, interruption of α-synuclein aggregation prevents neuronal degeneration in Parkinson's. Often such interactions are limited by insufficient concentrations of drugs reaching neuronal tissues and/or insufficient residence time of drug/s with the receptor. Hence, lipid nanoformulations, SLNs (solid lipid nanoparticles) and NLCs (nanostructured lipid carriers) emerged to overcome these challenges by utilizing physiological transport mechanisms across blood-brain barrier, such as drug-loaded SLN/NLCs adsorb apolipoproteins from the systemic circulation and are taken up by endothelial cells via low-density lipoprotein (LDL)-receptor mediated endocytosis and subsequently unload drugs at target site (neuronal tissue), which imparts selectivity, target ability, and reduction in toxicity. This paper reviews the utilization of SLN/NLCs as carriers for targeted delivery of novel CNS drugs to improve the clinical course of neurological disorders, placing some additional discussion on the metabolism of lipid-based formulations.

摘要

神经紊乱影响着全球数百万人,是造成残疾调整生命年(DALYs)的首要原因。目前的治疗方法多为对症治疗,且药物的作用往往受到内皮细胞层(由紧密连接蛋白连接;包括闭合蛋白、连接蛋白和连接黏附分子)、周细胞和星形足突构成的特殊网络的限制。近年来,纳米医学的发展使得通过改变信号机制(如在缺血性中风中激活 PI3K/Akt 通路以阻止细胞凋亡)来靶向治疗中枢神经系统(CNS)病理生物学的疗法成为可能,阻断α-突触核蛋白聚集可以防止帕金森病中的神经元退化。然而,这种相互作用往往受到药物到达神经元组织的浓度不足以及药物与受体的停留时间不足的限制。因此,脂质纳米制剂(SLN)、固体脂质纳米粒(SLN)和纳米结构脂质载体(NLC)的出现,通过利用跨越血脑屏障的生理转运机制(如载药 SLN/NLC 从全身循环中吸附载脂蛋白,并通过 LDL 受体介导的内吞作用被内皮细胞摄取,随后在靶部位(神经元组织)释放药物)来克服这些挑战,从而提高了药物的选择性、靶向能力和降低了毒性。本文综述了 SLN/NLC 作为新型 CNS 药物靶向递药载体的应用,以改善神经紊乱的临床病程,并对基于脂质的制剂的代谢进行了一些额外的讨论。

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