Unraveling the interaction between doxorubicin and DNA origami nanostructures for customizable chemotherapeutic drug release

6533b82dfe1ef96bd1290faf

RESEARCH PRODUCT

Unraveling the interaction between doxorubicin and DNA origami nanostructures for customizable chemotherapeutic drug release

Heini Ijäs Boxuan Shen Amelie Heuer-jungemann Adrian Keller Mauri A. Kostiainen Tim Liedl Janne A. Ihalainen Veikko Linko

subject

Drug Carriers Antibiotics Antineoplastic AcademicSubjects/SCI00010 organic chemicals technology industry and agriculture Magnesium Chloride lääkeaineet macromolecular substances DNA Buffers nanolääketiede Nanostructures carbohydrates (lipids)Drug Liberation nanorakenteet Chemical Biology and Nucleic Acid Chemistry Doxorubicin polycyclic compounds Deoxyribonuclease I

description

We thank Dr H. Häkkänen for technical assistance and S. Julin for the 24HB DNA origami design. We acknowledge the provision of facilities and technical support by Aalto University Bioeconomy Facilities and OtaNano – Nanomicroscopy Center (Aalto-NMC). The research was carried out under the Academy of Finland Centres of Excellence Programme (2014–2019). Academy of Finland [308578 to M.A.K.]; Deutsche Forschungsgemeinschaft [Emmy Noether Programme to A.H.-J., SFB1032 (Project A06) to T.L.]; Emil Aaltonen Foundation [to H.I. and V.L.]; Jane and Aatos Erkko Foundation [to J.A.I. and V.L.]; Sigrid Jusélius Foundation [to V.L.]; Vilho, Yrjö and Kalle Väisälä Foundation of the Finnish Academy of Science and Letters [to V.L.]. Funding for open access charge: Emil Aaltonen Foundation.Publisher Copyright: © The Author(s) 2021. Published by Oxford University Press on behalf of Nucleic Acids Research. Copyright: This record is sourced from MEDLINE/PubMed, a database of the U.S. National Library of Medicine Doxorubicin (DOX) is a common drug in cancer chemotherapy, and its high DNA-binding affinity can be harnessed in preparing DOX-loaded DNA nanostructures for targeted delivery and therapeutics. Although DOX has been widely studied, the existing literature of DOX-loaded DNA-carriers remains limited and incoherent. Here, based on an in-depth spectroscopic analysis, we characterize and optimize the DOX loading into different 2D and 3D scaffolded DNA origami nanostructures (DONs). In our experimental conditions, all DONs show similar DOX binding capacities (one DOX molecule per two to three base pairs), and the binding equilibrium is reached within seconds, remarkably faster than previously acknowledged. To characterize drug release profiles, DON degradation and DOX release from the complexes upon DNase I digestion was studied. For the employed DONs, the relative doses (DOX molecules released per unit time) may vary by two orders of magnitude depending on the DON superstructure. In addition, we identify DOX aggregation mechanisms and spectral changes linked to pH, magnesium, and DOX concentration. These features have been largely ignored in experimenting with DNA nanostructures, but are probably the major sources of the incoherence of the experimental results so far. Therefore, we believe this work can act as a guide to tailoring the release profiles and developing better drug delivery systems based on DNA-carriers. Peer reviewed

year	journal	country	edition	language
2021-01-01	Nucleic Acids Research

10.1093/nar/gkab097 http://europepmc.org/articles/PMC8034656