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Abstract
Biomolecular polyelectrolyte complexes can be formed between oppositely charged intrinsically disordered regions (IDRs) of proteins or between IDRs and nucleic acids. Highly charged IDRs are abundant in the nucleus, yet few have been functionally characterized. Here, we show that a positively charged IDR within the human ATP-dependent DNA helicase Q4 (RECQ4) forms coacervates with G-quadruplexes (G4s). We describe a three-step model of charge-driven coacervation by integrating equilibrium and kinetic binding data in a global numerical model. The oppositely charged IDR and G4 molecules form a complex in the solution that follows a rapid nucleation-growth mechanism leading to a dynamic equilibrium between dilute and condensed phases. We also discover a physical interaction with Replication Protein A (RPA) and demonstrate that the IDR can switch between the two extremes of the structural continuum of complexes. The structural, kinetic, and thermodynamic profile of its interactions revealed a dynamic disordered complex with nucleic acids and a static ordered complex with RPA protein. The two mutually exclusive binding modes suggest a regulatory role for the IDR in RECQ4 function by enabling molecular handoffs. Our study extends the functional repertoire of IDRs and demonstrates a role of polyelectrolyte complexes involved in G4 binding.
In this work, the authors report a three-step charge-driven coacervation model involving dynamic complexes between a positively charged IDR of human RECQ4 and G-quadruplexes. The IDR also interacts with Replication Protein A, implying RECQ4’s regulatory role.
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1 Masaryk University, CEITEC-Central European Institute of Technology, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956)
2 Masaryk University, National Centre for Biomolecular Research, Faculty of Science, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956); Masaryk University, Department of Biology, Faculty of Medicine, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956)
3 Masaryk University, Department of Biology, Faculty of Medicine, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956)
4 Masaryk University, National Centre for Biomolecular Research, Faculty of Science, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956)
5 University College London, Institute of Structural and Molecular Biology, London, UK (GRID:grid.83440.3b) (ISNI:0000000121901201); University College London, School of Pharmacy, London, UK (GRID:grid.83440.3b) (ISNI:0000 0001 2190 1201)
6 Masaryk University, CEITEC-Central European Institute of Technology, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956); Masaryk University, National Centre for Biomolecular Research, Faculty of Science, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956); Masaryk University, Department of Condensed Matter Physics, Faculty of Science, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956)
7 Masaryk University, Loschmidt Laboratories, Department of Experimental Biology and RECETOX, Faculty of Science, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956); St Anne’s University Hospital, International Clinical Research Center, Brno, Czech Republic (GRID:grid.412752.7) (ISNI:0000 0004 0608 7557)
8 Masaryk University, National Centre for Biomolecular Research, Faculty of Science, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956); Masaryk University, Department of Biology, Faculty of Medicine, Brno, Czech Republic (GRID:grid.10267.32) (ISNI:0000 0001 2194 0956); St Anne’s University Hospital, International Clinical Research Center, Brno, Czech Republic (GRID:grid.412752.7) (ISNI:0000 0004 0608 7557)