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首页> 外文期刊>Angewandte Chemie >Covalent Attachment of Cyclic TAT Peptides to GFP Results in Protein Delivery into Live Cells with Immediate Bioavailability
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Covalent Attachment of Cyclic TAT Peptides to GFP Results in Protein Delivery into Live Cells with Immediate Bioavailability

机译:环状TAT肽与GFP的共价结合导致蛋白质立即递送到活细胞中并具有生物利用度

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摘要

The delivery of free molecules into the cytoplasm and nucleus by using arginine-rich cell-penetrating peptides (CPPs) has been limited to small cargoes, while large cargoes such as proteins are taken up and trapped in endocytic vesicles. Based on recent work, in which we showed that the transduction efficiency of arginine-rich CPPs can be greatly enhanced by cyclization, the aim was to use cyclic CPPs to transport full-length proteins, in this study green fluorescent protein (GFP), into the cytosol of living cells. Cyclic and linear CPP-GFP conjugates were obtained by using azido-functionalized CPPs and an alkyne-functionalized GFP. Our findings reveal that the cyclic-CPP-GFP conjugates are internalized into live cells with immediate bioavailability in the cytosol and the nucleus, whereas linear CPP analogues do not confer GFP transduction. This technology expands the application of cyclic CPPs to the efficient transport of functional full-length proteins into live cells.
机译:通过使用富含精氨酸的细胞穿透肽(CPP),将游离分子传递到细胞质和细胞核中仅限于小货物,而大货物(例如蛋白质)则被吸收并捕获在胞吞小泡中。基于最近的工作,在该工作中我们表明,通过环化可以大大提高精氨酸富集的CPPs的转导效率,目的是使用环状CPPs将全长蛋白(本研究中的绿色荧光蛋白(GFP))转运至活细胞的胞浆。通过使用叠氮基官能化的CPP和炔烃官能化的GFP获得环状和线性CPP-GFP缀合物。我们的发现表明,环状CPP-GFP偶联物被内化到活细胞中,并在细胞质和细胞核中具有立即的生物利用度,而线性CPP类似物则不赋予GFP转导。这项技术将环状CPP的应用扩展到功能性全长蛋白向活细胞中的有效转运。

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