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通过折叠实现的肽内化:三螺旋细胞穿透肽

Peptide internalization enabled by folding: triple helical cell-penetrating peptides.

作者信息

Shinde Aparna, Feher Katie M, Hu Chloe, Slowinska Katarzyna

机构信息

Department of Chemistry and Biochemistry, California State University Long Beach, Long Beach, 90840, Canada.

出版信息

J Pept Sci. 2015 Feb;21(2):77-84. doi: 10.1002/psc.2725. Epub 2014 Dec 18.

Abstract

Cell-penetrating peptides (CPPs) are known as efficient transporters of molecular cargo across cellular membranes. Their properties make them ideal candidates for in vivo applications. However, challenges in the development of effective CPPs still exist: CPPs are often fast degraded by proteases and large concentration of CPPs required for cargo transporting can cause cytotoxicity. It was previously shown that restricting peptide flexibility can improve peptide stability against enzymatic degradation and limiting length of CPP peptide can lower cytotoxic effects. Here, we present peptides (30-mers) that efficiently penetrate cellular membranes by combining very short CPP sequences and collagen-like folding domains. The CPP domains are hexa-arginine (R6) or arginine/glycine (RRGRRG). Folding is achieved through multiple proline-hydroxyproline-glycine (POG [proline-hydroxyproline-glycine])n repeats that form a collagen-like triple helical conformation. The folded peptides with CPP domains are efficiently internalized, show stability against enzymatic degradation in human serum and have minimal toxicity. Peptides lacking correct folding (random coil) or CPP domains are unable to cross cellular membranes. These features make triple helical cell-penetrating peptides promising candidates for efficient transporters of molecular cargo across cellular membranes.

摘要

细胞穿透肽(CPPs)是已知的能够有效转运分子货物穿过细胞膜的载体。它们的特性使其成为体内应用的理想候选物。然而,在开发有效的CPPs方面仍然存在挑战:CPPs常常会被蛋白酶快速降解,并且货物运输所需的高浓度CPPs可能会导致细胞毒性。先前的研究表明,限制肽的柔韧性可以提高肽对酶降解的稳定性,而限制CPP肽的长度可以降低细胞毒性。在此,我们展示了一种肽(30聚体),它通过结合非常短的CPP序列和类胶原折叠结构域来有效地穿透细胞膜。CPP结构域是六聚精氨酸(R6)或精氨酸/甘氨酸(RRGRRG)。折叠是通过多个脯氨酸-羟脯氨酸-甘氨酸(POG [脯氨酸-羟脯氨酸-甘氨酸])n重复序列实现的,这些重复序列形成类胶原三螺旋构象。带有CPP结构域的折叠肽能够有效地内化,在人血清中对酶降解具有稳定性,并且毒性极小。缺乏正确折叠(无规卷曲)或CPP结构域的肽无法穿过细胞膜。这些特性使得三螺旋细胞穿透肽成为分子货物跨细胞膜高效转运的有前景的候选物。

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