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DNA 受限单分子层中限制酶对 DNA 的切割具有位点选择性。

Site accessibility tailors DNA cleavage by restriction enzymes in DNA confined monolayers.

机构信息

Elettra Sincrotrone Trieste, s.s. 14 km 163.5 in Area Science Park, Trieste, Italy.

出版信息

Nanoscale. 2017 May 18;9(19):6399-6405. doi: 10.1039/c7nr00966f.

Abstract

Density-tunable nanografted monolayers (NAMs) of short oligonucleotide sequences on gold surfaces show novel properties that make them suitable for advanced biosensing applications, and in particular to study the effects of crowding and confinement on biomolecular interactions. Here, combining atomic force microscopy nanolithography, topography measurements and coarse-grained molecular dynamics simulations, we investigated restriction enzyme reaction mechanisms within confined DNA brushes highlighting the role played by the DNA sequence conformation and restriction site position along the chain, respectively, in determining the accessibility of the enzyme, and its consequent cleavage efficiency.

摘要

金表面上短寡核苷酸序列的密度可调纳米接枝单层(NAMs)表现出新颖的性质,使它们适合于先进的生物传感应用,特别是用于研究拥挤和限制对生物分子相互作用的影响。在这里,我们结合原子力显微镜纳米光刻、形貌测量和粗粒度分子动力学模拟,研究了受限 DNA 刷内的限制性内切酶反应机制,突出了 DNA 序列构象和限制性位点在链上位置分别在确定酶的可及性及其随后的切割效率方面所起的作用。

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