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减弱的溶细胞肽诱导的膜通透性:通过皱襞细胞膜进入细胞内部的新概念。

Inducible Membrane Permeabilization by Attenuated Lytic Peptides: A New Concept for Accessing Cell Interiors through Ruffled Membranes.

机构信息

Institute for Chemical Research , Kyoto University , Uji, Kyoto 611-0011 , Japan.

出版信息

Mol Pharm. 2019 Jun 3;16(6):2540-2548. doi: 10.1021/acs.molpharmaceut.9b00156. Epub 2019 May 10.

DOI:10.1021/acs.molpharmaceut.9b00156
PMID:30945865
Abstract

A variety of mid-sized and large biomolecules have been used as tools to explore fundamental biological questions. However, such molecules are often cell-impermeable and thus unable to attain sufficient access to the cell interior. This inhibits their ability to yield analytical data about the cell interior or modify the cellular events. We have recently developed a peptide, engineered from a natural hemolytic peptide, named L17E. Substantial cytosolic delivery of biomacromolecules, including antibodies, was attained in the presence of this peptide. In this study, detailed analysis of the modes of action of L17E was conducted, elucidating that a large fraction of the cytosolic translocation of biomacromolecules is accomplished in the presence of L17E within 5 min. L17E stimulates actin polymerization and induces a dynamic structural alteration of cell membranes, resulting in a ruffled appearance. Studies using macropinocytosis inhibitors and proteins that control endosome maturation raise the possibility that the transient permeabilization of ruffled cell membranes, rather than the rupture of endosomal membranes, is the crucial mechanism for facile cytosolic translocation of biomacromolecules in the presence of L17E. Our results provide a distinct concept of intracellular delivery, different from direct translocation through cell membranes or endocytic uptake followed by endosomal escape. This method of permeabilization via membrane ruffling provides a novel concept in intracellular delivery.

摘要

已经有多种中大型生物分子被用作探索基本生物学问题的工具。然而,这些分子通常无法穿透细胞膜,因此无法充分进入细胞内部。这限制了它们获取细胞内部分析数据或改变细胞事件的能力。我们最近开发了一种肽,由天然溶血肽 L17E 工程化而来。在这种肽的存在下,可以实现生物大分子,包括抗体在内的大量细胞质内递呈。在这项研究中,我们详细分析了 L17E 的作用模式,结果表明,在 5 分钟内,大量生物大分子的细胞质内转运是在 L17E 的存在下完成的。L17E 刺激肌动蛋白聚合,并诱导细胞膜的动态结构改变,导致细胞膜起皱。使用巨胞饮抑制剂和控制内体成熟的蛋白质进行的研究提出了一种可能性,即在 L17E 的存在下,生物大分子易于细胞质内转运的关键机制是皱膜的瞬时通透性,而不是内体膜的破裂。我们的结果提供了一个与通过细胞膜直接转运或内吞摄取后再经内体逃逸不同的细胞内递呈的新概念。这种通过细胞膜皱襞的通透性方法为细胞内递呈提供了一个新的概念。

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