Selective drug delivery to the retinal cells: Biological barriers and avenues

药物输送 基因传递 视网膜 药品 药理学 生物利用度 视网膜 医学 遗传增强 神经科学 生物 纳米技术 眼科 生物化学 基因 材料科学
作者
Eva Ramsay,Tatu Lajunen,Madhushree Bhattacharya,Mika Reinisalo,Kirsi Rilla,Heidi Kidron,Tetsuya Terasaki,Arto Urtti
出处
期刊:Journal of Controlled Release [Elsevier BV]
卷期号:361: 1-19 被引量:7
标识
DOI:10.1016/j.jconrel.2023.07.028
摘要

Retinal drug delivery is a challenging, but important task, because most retinal diseases are still without any proper therapy. Drug delivery to the retina is hampered by the anatomical and physiological barriers resulting in minimal bioavailability after topical ocular and systemic administrations. Intravitreal injections are current method-of-choice in retinal delivery, but these injections show short duration of action for small molecules and low target bioavailability for many protein, gene based drugs and nanomedicines. State-of-art delivery systems are based on prolonged retention, controlled drug release and physical features (e.g. size and charge). However, drug delivery to the retina is not cell-specific and these approaches do not facilitate intracellular delivery of modern biological drugs (e.g. intracellular proteins, RNA based medicines, gene editing). In this focused review we highlight biological factors and mechanisms that form the basis for the selective retinal drug delivery systems in the future. Therefore, we are presenting current knowledge related to retinal membrane transporters, receptors and targeting ligands in relation to nanomedicines, conjugates, extracellular vesicles, and melanin binding. These issues are discussed in the light of retinal structure and cell types as well as future prospects in the field. Unlike in some other fields of targeted drug delivery (e.g. cancer research), selective delivery technologies have been rarely studied, even though cell targeted delivery may be even more feasible after local administration into the eye.

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