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In-vitro blood-brain barrier models for drug screening and permeation studies: an overview

机译:用于药物筛选和渗透研究的体外血脑屏障模型:概述

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The blood-brain barrier (BBB) is comprised of brain microvascular endothelial central nervous system (CNS) cells, which communicate with other CNS cells (astrocytes, pericytes) and behave according to the state of the CNS, by responding against pathological environments and modulating disease progression. The BBB plays a crucial role in maintaining homeostasis in the CNS by maintaining restricted transport of toxic or harmful molecules, transport of nutrients, and removal of metabolites from the brain. Neurological disorders, such as NeuroHIV, cerebral stroke, brain tumors, and other neurodegenerative diseases increase the permeability of the BBB. While on the other hand, semipermeable nature of BBB restricts the movement of bigger molecules i.e. drugs or proteins (500?kDa) across it, leading to minimal bioavailability of drugs in the CNS. This poses the most significant shortcoming in the development of therapeutics for CNS neurodegenerative disorders. Although the complexity of the BBB (dynamic and adaptable barrier) affects approaches of CNS drug delivery and promotes disease progression, understanding the composition and functions of BBB provides a platform for novel innovative approaches towards drug delivery to CNS. The methodical and scientific interests in the physiology and pathology of the BBB led to the development and the advancement of numerous in vitro models of the BBB. This review discusses the fundamentals of BBB structure, permeation mechanisms, an overview of all the different in-vitro BBB models with their advantages and disadvantages, and rationale of selecting penetration prediction methods towards the critical role in the development of the CNS therapeutics.
机译:血脑屏障(BBB)由大脑微血管内皮中枢神经系统(CNS)细胞组成,这些细胞与其他CNS细胞(星形细胞,周细胞)进行通讯,并通过对病理环境做出反应并进行调节,从而根据CNS的状态起作用疾病进展。 BBB通过限制有毒或有害分子的运输,营养物质的运输以及从大脑中清除代谢物,在维持中枢神经系统的稳态中起着至关重要的作用。神经系统疾病,例如NeuroHIV,脑中风,脑瘤和其他神经退行性疾病,会增加血脑屏障的通透性。另一方面,BBB的半渗透性限制了较大分子(即药物或蛋白质(> 500kkDa))通过其的运动,从而导致CNS中药物的生物利用度最小。这在中枢神经系统神经退行性疾病的治疗方法的开发中构成了最大的缺点。尽管BBB的复杂性(动态和适应性障碍)影响中枢神经系统药物递送的方法并促进疾病进展,但了解BBB的组成和功能为新型创新方法向中枢神经系统药物递送提供了平台。对BBB生理学和病理学的方法学和科学兴趣导致了BBB众多体外模型的发展和进步。这篇综述讨论了BBB结构的基本原理,渗透机制,所有不同的体外BBB模型的优缺点,以及选择针对中枢神经系统疗法发展中关键作用的渗透预测方法的原理。

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