The mechanisms by which intrinsically disordered proteins engage in rapid and highly selective binding is a subject of considerable interest and represents a central paradigmto nuclear porecomplex (NPC) function, where nuclear transport receptors (NTRs) move through the NPC by binding disordered phenylalanine- glycine-rich nucleoporins (FG-Nups). Combining single-molecule fluorescence, molecular simulations, and nuclear magnetic resonance, we show that a rapidly fluctuating FG-Nup populates an ensemble of conformations that are prone to bind NTRs with near diffusion-limited on rates, as shown by stopped-flow kinetic measurements. This is achieved using multiple, minimalistic, low-affinity binding motifs that are in rapid exchange when engaging with the NTR, allowing the FG-Nup to maintain an unexpectedly high plasticity in its bound state. We propose that these exceptional physical characteristics enable a rapid and specific transport mechanism in the physiological context, a notion supported by single molecule in-cell assays on intact NPCs.
Plasticity of an Ultrafast Interaction between Nucleoporins and Nuclear Transport Receptors / Milles, Sigrid; Mercadante, D; Aramburu Iker, Valle; Jensen Malene, Ringkjobing; Banterle, Niccolo; Koehler, Christine; Tyagi, Swati; Clarke, Jane; Shammas Sarah, L.; Blackledge, Martin; Graeter, Frauke; Lemke Edward, A.. - In: CELL. - ISSN 0092-8674. - 163:3(2015), pp. 734-745. [10.1016/j.cell.2015.09.047]
Plasticity of an Ultrafast Interaction between Nucleoporins and Nuclear Transport Receptors
Mercadante D;
2015
Abstract
The mechanisms by which intrinsically disordered proteins engage in rapid and highly selective binding is a subject of considerable interest and represents a central paradigmto nuclear porecomplex (NPC) function, where nuclear transport receptors (NTRs) move through the NPC by binding disordered phenylalanine- glycine-rich nucleoporins (FG-Nups). Combining single-molecule fluorescence, molecular simulations, and nuclear magnetic resonance, we show that a rapidly fluctuating FG-Nup populates an ensemble of conformations that are prone to bind NTRs with near diffusion-limited on rates, as shown by stopped-flow kinetic measurements. This is achieved using multiple, minimalistic, low-affinity binding motifs that are in rapid exchange when engaging with the NTR, allowing the FG-Nup to maintain an unexpectedly high plasticity in its bound state. We propose that these exceptional physical characteristics enable a rapid and specific transport mechanism in the physiological context, a notion supported by single molecule in-cell assays on intact NPCs.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
