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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Gramicidin A-based peptide vector for intracellular protein delivery.
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Gramicidin A-based peptide vector for intracellular protein delivery.

机译:基于Gramicidin A的用于细胞内蛋白质递送的肽载体。

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The development of the peptide-based vectors for the intracellular delivery of biologically active macromolecules has opened new prospects of their application in research and therapy. Earlier the amphipathic cell-penetrating peptide (CPP) Pep-1 was reported to mediate cellular uptake of proteins without covalent binding to them. In this work we studied the ability of a series of membrane-active amphipathic peptides, based on the gramicidin A sequence, to transport a model protein across the eukaryotic cell membrane. Among them the positively charged Cys-containing peptide P10C demonstrated the most effective beta-galactosidase intracellular delivery. Besides, this peptide was shown to form noncovalent associates with beta-galactosidase as judged from electrophoresis and enzymatic activity assays. In addition, a series of new gramicidin analogues were prepared and the effect of N-terminus modification of gramicidin on the protein transduction efficiency was studied.
机译:用于细胞内递送生物活性大分子的基于肽的载体的开发为它们在研究和治疗中的应用打开了新的前景。早先据报道,两亲性细胞穿透肽(CPP)Pep-1可以介导蛋白质的细胞摄取,而不会与它们共价结合。在这项工作中,我们研究了基于短杆菌肽A序列的一系列具有膜活性的两亲性肽在真核细胞膜上转运模型蛋白的能力。其中带正电的含Cys肽P10C表现出最有效的β-半乳糖苷酶细胞内递送。此外,从电泳和酶活性测定中判断,该肽显示出与β-半乳糖苷酶形成非共价缔合体。此外,制备了一系列新的短杆菌肽类似物,并研究了短杆菌肽的N末端修饰对蛋白质转导效率的影响。

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