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Niosome-Based Approach for In Situ Gene Delivery to Retina and Brain Cortex as Immune-Privileged Tissues

机译:基于Niosome的方法将原位基因作为免疫组织转移到视网膜和大脑皮层

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摘要

Non-viral vectors have emerged as a promising alternative to viral gene delivery systems due to their safer profile. Among non-viral vectors, recently, niosomes have shown favorable properties for gene delivery, including low toxicity, high stability, and easy production. The three main components of niosome formulations include a cationic lipid that is responsible for the electrostatic interactions with the negatively charged genetic material, a non-ionic surfactant that enhances the long-term stability of the niosome, and a helper component that can be added to improve its physicochemical properties and biological performance. This review is aimed at providing recent information about niosome-based non-viral vectors for gene delivery purposes. Specially, we will discuss the composition, preparation methods, physicochemical properties, and biological evaluation of niosomes and corresponding nioplexes that result from the addition of the genetic material onto their cationic surface. Next, we will focus on the in situ application of such niosomes to deliver the genetic material into immune-privileged tissues such as the brain cortex and the retina. Finally, as future perspectives, non-invasive administration routes and different targeting strategies will be discussed.
机译:非病毒载体由于其更安全的特性而已成为病毒基因递送系统的有前途的替代品。最近,在非病毒载体中,脂质体显示出有利于基因传递的特性,包括低毒性,高稳定性和易于生产。脂质体制剂的三个主要成分包括负责与带负电荷的遗传物质发生静电相互作用的阳离子脂质,增强脂质体长期稳定性的非离子表面活性剂以及可以添加到其中的辅助成分。改善其理化性质和生物学性能。这篇综述旨在提供有关基于脂质体的非病毒载体用于基因递送的最新信息。特别是,我们将讨论由遗传物质添加到阳离子表面上而产生的脂质体和相应的复合物的组成,制备方法,理化性质和生物学评估。接下来,我们将集中在这些脂质体的原位应用,以将遗传物质传递到免疫功能低下的组织中,例如大脑皮层和视网膜。最后,作为未来的观点,将讨论非侵入性管理途径和不同的靶向策略。

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