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DNA 折纸纳米结构的低温保存。

Cryopreservation of DNA Origami Nanostructures.

机构信息

Technical and Macromolecular Chemistry, Paderborn University, Warburger Str. 100, 33098, Paderborn, Germany.

Faculty of Physics and Center for NanoScience (CeNS), Ludwig-Maximilians-University, Geschwister-Scholl-Platz 1, 80539, Munich, Germany.

出版信息

Small. 2020 Apr;16(13):e1905959. doi: 10.1002/smll.201905959. Epub 2020 Mar 4.

Abstract

Although DNA origami nanostructures have found their way into numerous fields of fundamental and applied research, they often suffer from rather limited stability when subjected to environments that differ from the employed assembly conditions, that is, suspended in Mg -containing buffer at moderate temperatures. Here, means for efficient cryopreservation of 2D and 3D DNA origami nanostructures and, in particular, the effect of repeated freezing and thawing cycles are investigated. It is found that, while the 2D DNA origami nanostructures maintain their structural integrity over at least 32 freeze-thaw cycles, ice crystal formation makes the DNA origami gradually more sensitive toward harsh sample treatment conditions. Whereas no freeze damage could be detected in 3D DNA origami nanostructures subjected to 32 freeze-thaw cycles, 1000 freeze-thaw cycles result in significant fragmentation. The cryoprotectants glycerol and trehalose are found to efficiently protect the DNA origami nanostructures against freeze damage at concentrations between 0.2 × 10 and 200 × 10 m and without any negative effects on DNA origami shape. This work thus provides a basis for the long-term storage of DNA origami nanostructures, which is an important prerequisite for various technological and medical applications.

摘要

尽管 DNA 折纸纳米结构已经在基础研究和应用研究的众多领域得到了应用,但当它们处于与组装条件不同的环境中时,通常会受到相当大的限制,例如在含有镁的缓冲液中在中等温度下悬浮。在这里,研究了高效冷冻保存 2D 和 3D DNA 折纸纳米结构的方法,特别是反复冷冻和解冻循环的影响。结果发现,尽管 2D DNA 折纸纳米结构在至少 32 次冷冻-解冻循环中保持其结构完整性,但冰晶的形成使 DNA 折纸纳米结构对恶劣的样品处理条件更加敏感。虽然在经过 32 次冷冻-解冻循环的 3D DNA 折纸纳米结构中没有检测到冷冻损伤,但 1000 次冷冻-解冻循环会导致明显的碎片。发现甘油和海藻糖等冷冻保护剂在 0.2×10 到 200×10 m 的浓度范围内可以有效地保护 DNA 折纸纳米结构免受冷冻损伤,并且对 DNA 折纸纳米结构的形状没有任何负面影响。这项工作为 DNA 折纸纳米结构的长期存储提供了基础,这是各种技术和医疗应用的重要前提。

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