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基于DNA的结构自组装网络的自动化探索

Automated exploration of DNA-based structure self-assembly networks.

作者信息

Cazenille L, Baccouche A, Aubert-Kato N

机构信息

Department of Information Sciences, Ochanomizu University, Tokyo, Japan.

CIBIO, University of Trento, Povo, Italy.

出版信息

R Soc Open Sci. 2021 Oct 6;8(10):210848. doi: 10.1098/rsos.210848. eCollection 2021 Oct.

Abstract

Finding DNA sequences capable of folding into specific nanostructures is a hard problem, as it involves very large search spaces and complex nonlinear dynamics. Typical methods to solve it aim to reduce the search space by minimizing unwanted interactions through restrictions on the design (e.g. staples in DNA origami or voxel-based designs in DNA Bricks). Here, we present a novel methodology that aims to reduce this search space by identifying the relevant properties of a given assembly system to the emergence of various families of structures (e.g. simple structures, polymers, branched structures). For a given set of DNA strands, our approach automatically finds chemical reaction networks (CRNs) that generate sets of structures exhibiting ranges of specific user-specified properties, such as length and type of structures or their frequency of occurrence. For each set, we enumerate the possible DNA structures that can be generated through domain-level interactions, identify the most prevalent structures, find the best-performing sequence sets to the emergence of target structures, and assess CRNs' robustness to the removal of reaction pathways. Our results suggest a connection between the characteristics of DNA strands and the distribution of generated structure families.

摘要

寻找能够折叠成特定纳米结构的DNA序列是一个难题,因为这涉及到非常大的搜索空间和复杂的非线性动力学。解决该问题的典型方法旨在通过对设计进行限制(例如DNA折纸中的钉书针或DNA砖中的基于体素的设计)来最小化不必要的相互作用,从而减少搜索空间。在此,我们提出了一种新颖的方法,旨在通过识别给定组装系统对于各种结构家族(例如简单结构、聚合物、分支结构)出现的相关属性来减少此搜索空间。对于给定的一组DNA链,我们的方法会自动找到化学反应网络(CRN),这些网络会生成展现特定用户指定属性范围的结构集,例如结构长度和类型或其出现频率。对于每组结构,我们会枚举通过域级相互作用可生成的可能DNA结构,识别最普遍的结构,找到对于目标结构出现表现最佳的序列集,并评估CRN对反应途径去除的稳健性。我们的结果表明DNA链的特征与生成的结构家族分布之间存在联系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9f8d/8493194/e36643b20ce8/rsos210848f01.jpg

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