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大分子拥挤促进生物纳米孔内单链DNA捕获:尺寸变化和溶液异质性的作用

Macromolecular Crowding Facilitates ssDNA Capture within Biological Nanopores: Role of Size Variation and Solution Heterogeneity.

作者信息

Punia Bhawakshi, Chaudhury Srabanti

机构信息

Department of Chemistry, Indian Institute of Science Education and Research, Dr. Homi Bhabha Road, Pune 411008, Maharashtra, India.

出版信息

J Phys Chem B. 2024 Feb 29;128(8):1876-1883. doi: 10.1021/acs.jpcb.3c08350. Epub 2024 Feb 14.

Abstract

Genetic sequencing is a vital process that requires the transport of charged nucleic acids through transmembrane nanopores. Single-molecule studies show that macromolecular bulk crowding facilitates the capture of these polymers, leading to a high throughput of nanopore sensors. Motivated by these observations, a minimal discrete-state stochastic framework was developed to describe the role of poly(ethylene glycol) (PEG) crowders in varying concentrations in the transport of ssDNA through α-hemolysin nanopores. This theory suggested that the cooperative partitioning of polycationic PEGs controls the capture of ssDNA due to underlying electrostatic interactions. Herein, we investigate the impact of the size variation of PEGs on the capture event. Even though larger crowders attract ssDNA strongly to enhance its capture, our results show that considerable cooperative partitioning of PEGs is also required to achieve high interevent frequency. The exact analytical results are supported by existing single-molecule studies. Since real cellular conditions are heterogeneous, its influence on the ssDNA capture rate is studied by introducing a binary mixture of crowders. Our results indicate that the "polymer-pushing-polymer" concept possibly affects the capture rate depending on the mixture composition. These new findings provide valuable insights into the microscopic mechanism of the capture process, which eventually allows for accurate genome sequencing in crowded solutions.

摘要

基因测序是一个至关重要的过程,它需要带电核酸通过跨膜纳米孔进行转运。单分子研究表明,大分子的体积拥挤效应有助于捕获这些聚合物,从而实现纳米孔传感器的高吞吐量。受这些观察结果的启发,我们开发了一个最小离散状态随机框架,以描述不同浓度的聚乙二醇(PEG)拥挤剂在单链DNA通过α-溶血素纳米孔转运过程中的作用。该理论表明,由于潜在的静电相互作用,聚阳离子PEG的协同分配控制着单链DNA的捕获。在此,我们研究了PEG大小变化对捕获事件的影响。尽管较大的拥挤剂对单链DNA有很强的吸引力,从而增强其捕获能力,但我们的结果表明,PEG的大量协同分配对于实现高事件间频率也是必需的。现有的单分子研究支持了确切的分析结果。由于真实的细胞环境是异质的,因此我们通过引入拥挤剂的二元混合物来研究其对单链DNA捕获率的影响。我们的结果表明,“聚合物推动聚合物”的概念可能会根据混合物的组成影响捕获率。这些新发现为捕获过程的微观机制提供了有价值的见解,最终有助于在拥挤溶液中进行准确的基因组测序。

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