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首页> 外文期刊>International journal of molecular medicine >Isolation of novel cell-penetrating peptides from a random peptide library using in vitro virus and their modifications.
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Isolation of novel cell-penetrating peptides from a random peptide library using in vitro virus and their modifications.

机译:使用体外病毒及其修饰从随机肽库中分离出新型可穿透细胞的肽。

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摘要

A number of cell-penetrating peptides (CPPs) have been reported, but their transduction efficiencies are too low to be used as intracellular carriers for therapeutic purposes. We conducted a comprehensive search to find novel CPPs using an in vitro virus (IVV) library, which presented random peptides consisting of 15 amino acids (diversity of the library was >10(12)). We found 9 kinds of novel CPPs with an intracellular translocation efficiency higher than that of the TAT peptide (YGRKKKRRQRRR). Interestingly, one of the novel CPPs, No. 14 (KLWMRWYSPTTRRYG), showed a dramatic improvement in translocation activity relative to the TAT peptide in CHO cells (>10-fold efficiency in 50 microM). As the intracellular translocation efficiency of No. 14 was increased by substitution Arg for Lys1 (14-1), we carried out alanine scanning on the basis of 14-1 to determine important amino acids for the intracellular translocation. The Ala substitution analysis showed that both Arg and Trp residues were important for the cell-penetrating activity and that their contribution was in the order Trp3
机译:已经报道了许多细胞穿透肽(CPP),但是它们的转导效率太低而不能用作治疗目的的细胞内载体。我们进行了全面搜索,以使用体外病毒(IVV)文库查找新型CPP,该文库提供了由15个氨基酸组成的随机肽(文库的多样性> 10(12))。我们发现9种新型CPP,其细胞内转运效率高于TAT肽(YGRKKKRRQRRR)。有趣的是,一种新型CPP(第14号)(KLWMRWYSPTTRRYG)相对于TAT肽在CHO细胞中表现出了显着的转运活性提高(在50 microM中效率> 10倍)。由于通过用Arg取代Lys1(14-1)提高了14号的细胞内转运效率,我们在14-1的基础上进行了丙氨酸扫描,以确定用于细胞内转运的重要氨基酸。 Ala取代分析表明,Arg和Trp残基都对细胞穿透活性很重要,并且它们的贡献顺序为Trp3

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