4.7 Article

DNA Nanostructure-Programmed Like-Charge Attraction at the Cell-Membrane Interface

Journal

ACS CENTRAL SCIENCE
Volume 4, Issue 10, Pages 1344-1351

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acscentsci.8b00383

Keywords

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Funding

  1. National Key R&D Program of China [2016YFA0400900]
  2. National Natural Science Foundation of China [NSFC 21604060, 11474155, 11774147, 21675167, 31571014, U1532119, 21775157, 11575278, 21505148, 21390414]
  3. Chinese Academy of Sciences (Instrument Developing Project)
  4. Chinese Academy of Sciences (Open Large Infrastructure Research)
  5. Chinese Academy of Sciences (Key Research Program of Frontier Sciences) [QYZDJ-SSW-SLH031]

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Cell entry of anionic nano-objects has been observed in various types of viruses and self-assembled DNA nanostructures. Nevertheless, the physical mechanism underlying the internalization of these anionic particles across the negatively charged cell membrane remains poorly understood. Here, we report the use of virus-mimicking designer DNA nanostructures with near-atomic resolution to program like-charge attraction at the interface of cytoplasmic membranes. Single-particle tracking shows that cellular internalization of tetrahedral DNA nanostructures (TDNs) depends primarily on the lipid-raft-mediated pathway, where caveolin plays a key role in providing the short-range attraction at the membrane interface. Both simulation and experimental data establish that TDNs approach the membrane primarily with their corners to minimize electrostatic repulsion, and that they induce uneven charge redistribution in the membrane under the short-distance confinement by caveolin. We expect that the nanoscale like-charge attraction mechanism provides new clues for viral entry and general rules for rational design of anionic carriers for therapeutics.

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