4.5 Article

Sequence-Controlled Adhesion and Microemulsification in a Two-Phase System of DNA Liquid Droplets

Journal

JOURNAL OF PHYSICAL CHEMISTRY B
Volume 124, Issue 40, Pages 8888-8895

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/acs.jpcb.0c06911

Keywords

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Funding

  1. NSF MRSEC Program [DMR 1720256]
  2. U.S. Department of Energy (DOE), Office of Science, Basic Energy Sciences (BES) [DESC0014427]
  3. ONR [N00014-18-1-2649]
  4. NSF MRI [DBI-1625770]

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Membrane-less organelles, the liquid droplets formed via liquid-liquid phase separation (LLPS) of biomolecules in cells, act to organize intracellular components into multiple compartments. As a model for this process, and as a potential vehicle for in vitro exploitation of its properties, we explore here a synthetic multiphase LLPS system consisting of a mixture of self-assembled DNA particles. The particles, termed DNA nanostars (NSs), consist of four double-stranded DNA arms that each terminate in a single-stranded overhang. NSs condense into droplets due to overhang hybridization. Using two types of NSs with orthogonal overhangs enables the creation of two types of immiscible DNA droplets. Adhesion between the droplets can be tuned by the addition of cross-linker NSs that have two overhang sequences of each type. We find that increasing the amount of the cross-linker NSs decreases the droplet/droplet surface tension until a microemulsion transition occurs. Controlled droplet adhesion can also be achieved, without cross-linkers, using overhangs that can weakly hybridize. Finally, we show that solutes can be specifically targeted to the DNA phases by labeling them with appropriate sticky-ends. Overall, our findings demonstrate the ability to create a multiphase LLPS system, and to control its mesoscale configuration, via sequence design of the component molecules.

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