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Arginine-rich cell-penetrating peptide-modified extracellular vesicles for active macropinocytosis induction and efficient intracellular delivery

机译:富精氨酸的细胞穿透肽修饰的细胞外囊泡用于主动诱导巨胞饮作用和有效的细胞内递送

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摘要

Extracellular vesicles (EVs) including exosomes have been shown to play crucial roles in cell-to-cell communication because of their ability to carry biofunctional molecules (e.g., microRNAs and enzymes). EVs also have pharmaceutical advantages and are highly anticipated to be a next-generation intracellular delivery tool. Here, we demonstrate an experimental technique that uses arginine-rich cell-penetrating peptide (CPP)-modified EVs to induce active macropinocytosis for effective cellular EV uptake. Modification of arginine-rich CPPs on the EV membrane resulted in the activation of the macropinocytosis pathway, and the number of arginine residues in the peptide sequences affected the cellular EV uptake efficiency. Consequently, the ribosome-inactivating protein saporin-encapsulated EVs modified with hexadeca-arginine (R16) peptide effectively attained anti-cancer activity.
机译:包括外泌体的细胞外囊泡(EV)已被证明在细胞间通信中起着至关重要的作用,因为它们具有携带生物功能分子(例如microRNA和酶)的能力。电动汽车也具有药学优势,并且被高度期待成为下一代细胞内递送工具。在这里,我们演示了一种实验技术,该技术使用富含精氨酸的细胞穿透肽(CPP)修饰的EV诱导有效的细胞EV摄取的主动大胞饮作用。 EV膜上富含精氨酸的CPP的修饰导致巨胞饮途径的激活,并且肽序列中精氨酸残基的数量影响细胞的EV吸收效率。因此,用十六烷基精氨酸(R16)肽修饰的核糖体失活蛋白皂草苷包裹的电动汽车有效地获得了抗癌活性。

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