Programming crystallization kinetics of self-assembled DNA crystals with 5-methylcytosine modification

Author:

Chen Jielin1ORCID,Dai Zheze1,Lv Hui12,Jin Zhongchao1,Tang Yuqing1,Xie Xiaodong1,Shi Jiye3ORCID,Wang Fei1,Li Qian1,Liu Xiaoguo1ORCID,Fan Chunhai1ORCID

Affiliation:

1. School of Chemistry and Chemical Engineering, New Cornerstone Science Laboratory, Frontiers Science Center for Transformative Molecules and National Center for Translational Medicine, Shanghai Jiao Tong University, Shanghai 200240, China

2. Zhangjiang Laboratory, Shanghai 201210, China

3. Division of Physical Biology, Key Laboratory of Interfacial Physics and Technology, Shanghai Institute of Applied Physics, Chinese Academy of Sciences, Shanghai 201800, China

Abstract

Self-assembled DNA crystals offer a precise chemical platform at the ångström-scale for DNA nanotechnology, holding enormous potential in material separation, catalysis, and DNA data storage. However, accurately controlling the crystallization kinetics of such DNA crystals remains challenging. Herein, we found that atomic-level 5-methylcytosine (5mC) modification can regulate the crystallization kinetics of DNA crystal by tuning the hybridization rates of DNA motifs. We discovered that by manipulating the axial and combination of 5mC modification on the sticky ends of DNA tensegrity triangle motifs, we can obtain a series of DNA crystals with controllable morphological features. Through DNA-PAINT and FRET-labeled DNA strand displacement experiments, we elucidate that atomic-level 5mC modification enhances the affinity constant of DNA hybridization at both the single-molecule and macroscopic scales. This enhancement can be harnessed for kinetic-driven control of the preferential growth direction of DNA crystals. The 5mC modification strategy can overcome the limitations of DNA sequence design imposed by limited nucleobase numbers in various DNA hybridization reactions. This strategy provides a new avenue for the manipulation of DNA crystal structure, valuable for the advancement of DNA and biomacromolecular crystallography.

Funder

the National Nature Science Foundation of China

the National Nature Science Founation of China

the National Research Programs from the Ministry of Science and Technology of China

the National Key R&D Program of China

the China Postdoctoral Science Foundation

Publisher

Proceedings of the National Academy of Sciences

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