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首页> 外文期刊>Nanotechnology >An engineered coiled-coil polypeptide assembled onto quantum dots for targeted cell imaging
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An engineered coiled-coil polypeptide assembled onto quantum dots for targeted cell imaging

机译:组装在量子点上的工程化卷曲螺旋多肽,用于靶向细胞成像

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摘要

Quantum dot (QD)-polypeptide probes have been developed through the specific metal-affinity interaction between polypeptides appended with N-terminal polyhistidine sequences and CdSe/ZnS core-shell QDs. The size and charge of a QD-polypeptide can be tuned by using different coiled-coil polypeptides. Compared to glutathione-capped QDs (QD-GSH), QD-polypeptide probes showed an approximately two-to three-fold luminescence increase, and the luminescence increase was not obviously related to the charge of the polypeptide. QD-polypeptide probes with different charge have a great effect on nonspecific cellular uptake. QD-polypeptide probes with negative charge exhibited lower nonspecific cellular uptake in comparison to the QD-GSH, while positively charged QD-polypeptide probes presented higher cellular uptake than the QD-GSH. A targeted QD-ARGD probe can obviously increase targeted cellular uptake in alpha(v)beta(3) overexpressing HeLa cells compared to QD-A. In addition, QD-polypeptide probes showed lower in vitro cytotoxicity compared to the original QDs. These results demonstrate that these QD-polypeptide probes with high specific cellular uptake, high fluorescence intensity and low background noise are expected to have great potential applications in targeted cell imaging.
机译:通过附加N端多组氨酸序列的多肽与CdSe / ZnS核-壳QD之间的特异性金属亲和相互作用,开发了量子点(QD)-多肽探针。 QD多肽的大小和电荷可以通过使用不同的卷曲螺旋多肽来调节。与带有谷胱甘肽的QD(QD-GSH)相比,QD多肽探针显示出大约2到3倍的发光增加,并且发光增加与多肽的电荷没有明显关系。带不同电荷的QD多肽探针对非特异性细胞摄取有很大影响。与QD-GSH相比,带负电荷的QD多肽探针显示出较低的非特异性细胞摄取,而带正电荷的QD-多肽探针显示的细胞摄取高于QD-GSH。与QD-A相比,靶向QD-ARGD探针可以明显增加过表达alpha(v)beta(3)的HeLa细胞的靶向细胞摄取。此外,与原始QD相比,QD多肽探针显示出更低的体外细胞毒性。这些结果表明,这些具有高特异性细胞摄取,高荧光强度和低背景噪音的QD多肽探针有望在靶向细胞成像中具有巨大的潜在应用。

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