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Differential interactions determine anisotropies at interfaces of RNA-based biomolecular condensates.

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Peer-reviewed

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Abstract

Biomolecular condensates form via macromolecular phase separation. Here, we report results from our characterization of synthetic condensates formed by phase separation of mixtures comprising two types of RNA molecules and the biocompatible polymer polyethylene glycol. Purine-rich RNAs are scaffolds that drive phase separation via heterotypic interactions. Conversely, pyrimidine-rich RNA molecules are adsorbents defined by weaker heterotypic interactions. They adsorb onto and wet the interfaces of coexisting phases formed by scaffolds. Lattice-based simulations reproduce the phenomenology observed in experiments and these simulations predict that scaffolds and adsorbents have different non-random orientational preferences at interfaces. Dynamics at interfaces were probed using single-molecule tracking of fluorogenic probes bound to RNA molecules. These experiments revealed dynamical anisotropy at interfaces whereby motions of probe molecules parallel to the interface are faster than motions perpendicular to the interface. Taken together, our findings have broad implications for designing synthetic condensates with tunable interfacial properties.

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Acknowledgements: This work was funded by an EMBO fellowship (ALTF 772-2024, N.A.E.), the Royall Scholarship (N.A.E.), the Center for Biomolecular Condensates at Washington University in St. Louis (N.A.E., R.V.P.), the European Union’s Horizon 2020 research and innovation program under the Marie Skłodowska-Curie grant MicroREvolution (agreement no. 101023060; T.S.), the Winston Churchill Foundation of the United States (T.J.W.), the Harding Distinguished Postgraduate Scholar Program (T.J.W.), Global Research Technologies Novo Nordisk A/S (H.A., T.P.J.K.), the US National Institutes of Health (R01NS121114 to R.V.P and R35GM124858 to M.D.L), the US Air Force Office of Scientific Research (FA9550-20-1-0241 R.V.P), the European Research Council under the European Union’s Seventh Framework Program (FP7/2007−2013) through the ERC grants PhysProt (agreement no. 337969; T.P.J.K.) and the Newman Foundation (T.P.J.K., T.S.).

Journal Title

Nat Commun

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Journal ISSN

2041-1723
2041-1723

Volume Title

16

Publisher

Springer Nature

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Except where otherwised noted, this item's license is described as http://creativecommons.org/licenses/by-nc-nd/4.0/
Sponsorship
European Research Council (337969)
European Commission Horizon 2020 (H2020) Marie Sk?odowska-Curie actions (101023060)