Delivery of RNA Therapeutics: The Great Endosomal Escape!

内体 小干扰RNA RNA干扰 寡核苷酸 核糖核酸 RNA沉默 内吞作用 细胞生物学 细胞 计算生物学 生物 基因 遗传学 细胞内
作者
Steven F. Dowdy,Ryan L. Setten,Xian-Shu Cui,Satish Jadhav
出处
期刊:Nucleic Acid Therapeutics [Mary Ann Liebert, Inc.]
卷期号:32 (5): 361-368 被引量:74
标识
DOI:10.1089/nat.2022.0004
摘要

RNA therapeutics, including siRNAs, antisense oligonucleotides, and other oligonucleotides, have great potential to selectively treat a multitude of human diseases, from cancer to COVID to Parkinson's disease. RNA therapeutic activity is mechanistically driven by Watson-Crick base pairing to the target gene RNA without the requirement of prior knowledge of the protein structure, function, or cellular location. However, before widespread use of RNA therapeutics becomes a reality, we must overcome a billion years of evolutionary defenses designed to keep invading RNAs from entering cells. Unlike small-molecule therapeutics that are designed to passively diffuse across the cell membrane, macromolecular RNA therapeutics are too large, too charged, and/or too hydrophilic to passively diffuse across the cellular membrane and are instead taken up into cells by endocytosis. However, similar to the cell membrane, endosomes comprise a lipid bilayer that entraps 99% or more of RNA therapeutics, even in semipermissive tissues such as the liver, central nervous system, and muscle. Consequently, before RNA therapeutics can achieve their ultimate clinical potential to treat widespread human disease, the rate-limiting delivery problem of endosomal escape must be solved in a clinically acceptable manner.
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