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细胞穿透肽进入脂质双分子层囊泡和细菌细胞的基本过程。

Elementary processes for the entry of cell-penetrating peptides into lipid bilayer vesicles and bacterial cells.

机构信息

Department of Biotechnology and Genetic Engineering, Jahangirnagar University, Savar, Dhaka, 1342, Bangladesh.

Integrated Bioscience Section, Graduate School of Science and Technology, Shizuoka University, Shizuoka, 422-8529, Japan.

出版信息

Appl Microbiol Biotechnol. 2018 May;102(9):3879-3892. doi: 10.1007/s00253-018-8889-5. Epub 2018 Mar 9.

Abstract

Cell-penetrating peptides (CPPs) can translocate across the plasma membrane of living eukaryotic cells and enter the cytosol without significantly affecting cell viability. Consequently, CPPs have been used for the intracellular delivery of biological cargo such as proteins and oligonucleotides. However, the mechanisms underlying the translocation of CPPs across the plasma membrane remain unclear. In this mini-review, we summarize the experimental results regarding the entry of CPPs into lipid bilayer vesicles obtained using three methods: the large unilamellar vesicle (LUV) suspension method, the giant unilamellar vesicle (GUV) suspension method, and the single GUV method. The advantages and disadvantages of these methods are also discussed. Experimental results to date clearly indicate that CPPs can translocate across lipid bilayers and enter the vesicle lumen. Three models for the mechanisms and pathways by which CPPs translocate across lipid bilayers are described: (A) through pores induced by CPPs, (B) through transient prepores, and (C) via formation of inverted micelles. Both the pathway of translocation and the efficiency of entry of CPPs depend on the lipid composition of the bilayer and the type of CPP. We also describe the interaction of CPPs with bacterial cells. Some CPPs have strong antimicrobial activities. There are two modes of action of CPPs on bacterial cells: CPPs can induce damage to the plasma membrane and thus increase permeability, or CPPs enter the cytosol of bacterial cells without damaging the plasma membrane. The information currently available on the elementary processes by which CPPs enter lipid bilayer vesicles and bacterial cells is valuable for elucidating the mechanisms of entry of CPPs into the cytosol of various eukaryotic cells.

摘要

细胞穿透肽 (CPP) 能够穿透活真核细胞的质膜并进入细胞质,而不会显著影响细胞活力。因此,CPP 已被用于生物货物(如蛋白质和寡核苷酸)的细胞内递送。然而,CPP 穿越质膜的转运机制仍不清楚。在这篇迷你综述中,我们总结了使用三种方法(大单层囊泡 (LUV) 悬浮法、巨大单层囊泡 (GUV) 悬浮法和单个 GUV 法)获得的 CPP 进入脂质双层囊泡的实验结果。还讨论了这些方法的优缺点。迄今为止的实验结果清楚地表明,CPP 可以穿透脂质双层并进入囊泡腔。描述了 CPP 穿越脂质双层的机制和途径的三种模型:(A) 通过 CPP 诱导的孔,(B) 通过瞬时前孔,和 (C) 通过形成反胶束。CPP 穿越的途径和进入效率取决于双层的脂质组成和 CPP 的类型。我们还描述了 CPP 与细菌细胞的相互作用。一些 CPP 具有很强的抗菌活性。CPP 对细菌细胞有两种作用模式:CPP 可以诱导质膜损伤从而增加通透性,或者 CPP 不破坏质膜而进入细菌细胞的细胞质。目前关于 CPP 进入脂质双层囊泡和细菌细胞的基本过程的信息对于阐明 CPP 进入各种真核细胞质的机制很有价值。

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