作者
Sanjay G Patel, Edward J Sayers, Lin He, Rohan Narayan, Thomas L Williams, Emily M Mills, Rudolf K Allemann, Louis YP Luk, Arwyn T Jones, Yu-Hsuan Tsai
发表日期
2019/4/18
期刊
Scientific reports
卷号
9
期号
1
页码范围
6298
出版商
Nature Publishing Group UK
简介
Protein therapy holds great promise for treating a variety of diseases. To act on intracellular targets, therapeutic proteins must cross the plasma membrane. This has previously been achieved by covalent attachment to a variety of cell-penetrating peptides (CPPs). However, there is limited information on the relative performance of CPPs in delivering proteins to cells, specifically the cytosol and other intracellular locations. Here we use green fluorescent protein (GFP) as a model cargo to compare delivery capacity of five CPP sequences (Penetratin, R8, TAT, Transportan, Xentry) and cyclic derivatives in different human cell lines (HeLa, HEK, 10T1/2, HepG2) representing different tissues. Confocal microscopy analysis indicates that most fusion proteins when incubated with cells at 10 µM localise to endosomes. Quantification of cellular uptake by flow cytometry reveals that uptake depends on both cell type (10T1/2 …
引用总数
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