Breaking the cellular delivery bottleneck: recent developments in direct cytosolic delivery of biologics.

Harini Nagaraj, Victor Lehot, Nourina Nasim, Yagiz Anil Cicek, Ritabrita Goswami, Taewon Jeon, Vincent M Rotello
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Abstract

Proteins and nucleic acid therapeutics represent a significant and growing share of the pharmaceutical landscape. The majority of biological and therapeutic applications of these biomolecules require access to the cytosol. Delivery of biologics directly to the cytosol is made difficult by the impermeability of the cell membrane. As a result, most delivery strategies have utilized endocytic uptake pathways to deliver biologics into the cell. However, endosomally entrapped cargo often faces limited escape efficiency and is prone to degradation within endo/lysosomal compartments. The emergence of delivery vehicles capable of bypassing endocytosis and directly traversing the cell membrane offers a promising approach to improve the cytosolic delivery efficiency of biomolecules. Here, we highlight recent developments in endocytosis-independent delivery systems for biologics and ways to accurately assess cytosolic delivery of biologics. Strategies employing covalent and non-covalent modification of biomolecules will be reviewed, along with strategies incorporating both covalent and supramolecular processes.

打破细胞递送瓶颈:生物制剂直接细胞质递送的最新进展。
蛋白质和核酸疗法在制药领域中占有重要的、不断增长的份额。这些生物分子的大多数生物学和治疗应用都需要进入细胞质。由于细胞膜的不渗透性,将生物制剂直接输送到细胞质中变得困难。因此,大多数递送策略利用内吞摄取途径将生物制剂递送到细胞中。然而,内体包裹的货物通常面临有限的逃逸效率,并且易于在内酶/溶酶体隔室内降解。能够绕过胞吞作用并直接穿过细胞膜的递送载体的出现为提高生物分子的胞质递送效率提供了一种有希望的方法。在这里,我们重点介绍了生物制剂的内吞非依赖性递送系统的最新进展,以及准确评估生物制剂的细胞质递送的方法。将回顾采用共价和非共价修饰生物分子的策略,以及结合共价和超分子过程的策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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