Cationic PTD/CPP-mediated macromolecular delivery: charging into the cell

内吞作用 内体 内化 高分子 转导(生物物理学) 细胞内 细胞穿透肽 细胞 细胞生物学 化学 生物 生物物理学 生物化学
作者
Peter Lönn,Steven F. Dowdy
出处
期刊:Expert Opinion on Drug Delivery [Taylor & Francis]
卷期号:12 (10): 1627-1636 被引量:124
标识
DOI:10.1517/17425247.2015.1046431
摘要

Introduction: Macromolecular therapeutics, including enzymes, transcription factors, siRNAs, peptides and large synthetic molecules, can potentially be used to treat human diseases by targeting intracellular molecular pathways and modulating biological responses. However, large macromolecules have no ability to enter cells and require delivery vehicles. Protein transduction domains (PTDs), also known as cell-penetrating peptides (CPPs), are a diverse class of peptides that can deliver macromolecules into cells.Areas covered: In this review, we cover the uptake and usage of arginine-rich PTDs/CPPs (TAT-PTD, Penetratin/Antp and 8R). We review the endocytosis-mediated uptake of these peptides and highlight three important steps: i) cell association; ii) internalization and iii) endosomal escape. We also discuss the array of different cargos that have been delivered by cationic PTDs/CPPs as well as cellular processes and biological responses that have been modulated.Expert opinion: PTDs/CPPs have shown great potential to deliver otherwise undeliverable macromolecular therapeutics into cells for experimentation in cell culture and in animal disease models in vivo. Moreover, over 25 clinical trials have been performed predominantly using the TAT-PTD. However, more work is still needed. Endosomal escape and target-cell specificity remain two of the major future challenges.
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