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Folding of single-stranded circular DNA into rigid rectangular DNA accelerates its cellular uptake

机译:折叠的单股的环状DNA为刚性矩形DNA加速细胞吸收

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摘要

Despite the importance of the interaction between DNA and cells for its biological activity, little is known about exactly how DNA interacts with cells. To elucidate the relationship between the structural properties of DNA and its cellular uptake, a single-stranded circular DNA of 1801 bases was designed and folded into a series of rectangular DNA (RecDNA) nanostructures with different rigidities using DNA origami technology. Interactions between these structures and cells were evaluated using mouse macrophage-like RAW264.7 cells. RecDNA with 50 staple DNAs, including four that were Alexa Fluor 488-labeled, was designed. RecDNA with fewer staples, down to four staples (all Alexa Fluor 488-labeled), was also prepared. Electrophoresis and atomic force microscopy showed that all DNA nanostructures were successfully obtained with a sufficiently high yield. Flow cytometry analysis showed that folding of the single-stranded circular DNA into RecDNA significantly increased its cellular uptake. In addition, there was a positive correlation between uptake and the number of staples. These results indicate that highly folded DNA nanostructures interact more efficiently with RAW264.7 cells than loosely folded structures do. Based on these results, it was concluded that the interaction of DNA with cells can be controlled by folding using DNA origami technology.
机译:尽管之间的交互的重要性DNA和细胞生物活性,很少已知DNA相互作用如何呢细胞。DNA和细胞结构的性质吸收,单链环状DNA的1801基地和折叠成一系列的设计矩形DNA (RecDNA)纳米结构不同的刚性使用DNA折纸技术。使用鼠标和细胞进行评估macrophage-like RAW264.7细胞。主要dna,包括四个Alexa萤石488 -标签,设计。斯台普斯,四个主食(Alexa萤石488 -标签),也准备好了。原子力显微镜显示所有的DNA纳米结构是成功了足够高的收益。表明,单链的折叠环状DNA进入RecDNA显著增加其细胞吸收。之间的正相关和吸收斯台普斯。高度折叠DNA纳米结构更多的互动效率比松散RAW264.7细胞折叠结构。是认为DNA之间的相互作用细胞可以控制使用DNA折叠折纸技术。

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