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一种使用基于质粒展示的功能选择平台鉴定的非寻常细胞穿透肽。

An unusual cell penetrating peptide identified using a plasmid display-based functional selection platform.

机构信息

Department of Chemical Engineering, Columbia University, New York, New York 10027, USA.

出版信息

ACS Chem Biol. 2011 May 20;6(5):484-91. doi: 10.1021/cb100423u. Epub 2011 Feb 22.

Abstract

Cell penetrating peptides (CPPs) have tremendous potential for use in gene and drug delivery applications. The selection of new CPPs with desired capabilities from randomized peptide libraries is challenging, since the CPP phenotype is a complex selection target. Here we report the discovery of an unusual new CPP from a randomized peptide library using a functional selection system based on plasmid display (PD). After four rounds of screening of a 14-mer peptide library over PC12 cells, several peptides were identified and tested for their ability to deliver the green fluorescent protein (GFP). One peptide (SG3) exhibited a cell penetrating phenotype; however, unlike other well-known CPPs such as TAT or Penetratin, the newly identified peptide was not highly cationic. The PD protocol necessitated the addition of a cationic lipid (Lipofectamine2000), and in the presence of this compound, the SG3 peptide significantly outperformed the well-known TAT CPP in the delivery of GFP to PC12 cells and primary astrocytes. When the SG3 peptide was fused to the pro-apoptotic BH3 peptide from the Bak protein, significant cell death was induced in cultured primary astrocytes, indicating relevant, intracellular delivery of a functional cargo. The PD platform is a useful method for identifying functional new CPPs from randomized libraries with unique delivery capabilities.

摘要

细胞穿透肽 (CPP) 在基因和药物传递应用中具有巨大的潜力。从随机肽文库中选择具有所需功能的新型 CPP 具有挑战性,因为 CPP 表型是一个复杂的选择目标。在这里,我们报告了一种使用基于质粒展示 (PD) 的功能选择系统从随机肽文库中发现的一种不寻常的新型 CPP。在经过四轮对 PC12 细胞的 14 肽文库的筛选后,鉴定出了几种肽,并测试了它们携带绿色荧光蛋白 (GFP) 的能力。一种肽 (SG3) 表现出细胞穿透表型;然而,与其他著名的 CPP 如 TAT 或 Penetratin 不同,新鉴定的肽不是高度阳离子的。PD 方案需要添加阳离子脂质 (Lipofectamine2000),并且在存在这种化合物的情况下,SG3 肽在将 GFP 递送至 PC12 细胞和原代星形胶质细胞中的性能明显优于著名的 TAT CPP。当 SG3 肽与来自 Bak 蛋白的促凋亡 BH3 肽融合时,在培养的原代星形胶质细胞中诱导了显著的细胞死亡,表明功能性货物的相关细胞内递送。PD 平台是一种从具有独特传递能力的随机文库中识别功能性新型 CPP 的有用方法。

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