内体
小干扰RNA
基因敲除
胞浆
内吞作用
细胞生物学
RNA干扰
基因沉默
生物
核糖核酸
细胞
生物化学
基因
细胞内
酶
作者
Anders Wittrup,Angela Ai,Xing Liu,Péter Hamar,Radiana Trifonova,Klaus Charissé,Muthiah Manoharan,Tomas Kirchhausen,Judy Lieberman
摘要
Live-cell imaging provides new insights in the cytosolic release mechanismsof lipid-formulated siRNAs. A central hurdle in developing small interfering RNAs (siRNAs) as therapeutics is the inefficiency of their delivery across the plasma and endosomal membranes to the cytosol, where they interact with the RNA interference machinery. With the aim of improving endosomal release, a poorly understood and inefficient process, we studied the uptake and cytosolic release of siRNAs, formulated in lipoplexes or lipid nanoparticles, by live-cell imaging and correlated it with knockdown of a target GFP reporter. siRNA release occurred invariably from maturing endosomes within ∼5–15 min of endocytosis. Cytosolic galectins immediately recognized the damaged endosome and targeted it for autophagy. However, inhibiting autophagy did not enhance cytosolic siRNA release. Gene knockdown occurred within a few hours of release and required <2,000 copies of cytosolic siRNAs. The ability to detect cytosolic release of siRNAs and understand how it is regulated will facilitate the development of rational strategies for improving the cytosolic delivery of candidate drugs.
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