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基于 DNA 的离子通道的膜活性取决于其双链结构的稳定性。

Membrane Activity of a DNA-Based Ion Channel Depends on the Stability of Its Double-Stranded Structure.

机构信息

Cavendish Laboratory, University of Cambridge, JJ Thomson Avenue, Cambridge, CB3 0HE, United Kingdom.

Department of Physics, University of Illinois at Urbana-Champaign, 1110 West Green Street, Urbana, Illinois 61801, United States.

出版信息

Nano Lett. 2021 Nov 24;21(22):9789-9796. doi: 10.1021/acs.nanolett.1c03791. Epub 2021 Nov 12.

Abstract

DNA nanotechnology has emerged as a promising method for designing spontaneously inserting and fully controllable synthetic ion channels. However, both insertion efficiency and stability of existing DNA-based membrane channels leave much room for improvement. Here, we demonstrate an approach to overcoming the unfavorable DNA-lipid interactions that hinder the formation of a stable transmembrane pore. Our all-atom MD simulations and experiments show that the insertion-driving cholesterol modifications can cause fraying of terminal base pairs of nicked DNA constructs, distorting them when embedded in a lipid bilayer. Importantly, we show that DNA nanostructures with no backbone discontinuities form more stable conductive pores and insert into membranes with a higher efficiency than the equivalent nicked constructs. Moreover, lack of nicks allows design and maintenance of membrane-spanning helices in a tilted orientation within the lipid bilayer. Thus, reducing the conformational degrees of freedom of the DNA nanostructures enables better control over their function as synthetic ion channels.

摘要

DNA 纳米技术已成为设计自发插入和完全可控的合成离子通道的一种很有前途的方法。然而,现有的基于 DNA 的膜通道的插入效率和稳定性还有很大的改进空间。在这里,我们展示了一种克服阻碍形成稳定跨膜孔的不利 DNA-脂质相互作用的方法。我们的全原子 MD 模拟和实验表明,插入驱动的胆固醇修饰会导致切口 DNA 结构的末端碱基对磨损,当它们嵌入脂质双层时会使它们变形。重要的是,我们表明,与等效的切口构建体相比,没有骨架不连续性的 DNA 纳米结构形成更稳定的导电孔,并以更高的效率插入膜中。此外,没有切口可以允许在脂质双层内以倾斜的取向设计和维持跨膜螺旋。因此,减少 DNA 纳米结构的构象自由度可以更好地控制它们作为合成离子通道的功能。

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