Abstract
There is a growing recognition for the importance of proteins with large intrinsically disordered (ID) segments in cell signaling and regulation. ID segments in these proteins often harbor regions that mediate molecular recognition. Coupled folding and binding of the recognition regions has been proposed to confer high specificity to interactions involving ID segments. However, researchers recently questioned the origin of the interaction specificity of ID proteins because of the overrepresentation of hydrophobic residues in their interaction interfaces. Here, we focused on the role of polar and charged residues in interactions mediated by ID segments. Making use of the extended nature of most ID segments when in complex with globular proteins, we first identified large numbers of complexes between globular proteins and ID segments by using radius-of-gyration-based selection criteria. Consistent with previous studies, we found the interfaces of these complexes to be enriched in hydrophobic residues, and that these residues contribute significantly to the stability of the interaction interface. However, our analyses also show that polar interactions play a larger role in these complexes than in structured protein complexes. Computational alanine scanning and salt-bridge analysis indicate that interfaces in ID complexes are highly complementary with respect to electrostatics, more so than interfaces of globular proteins. Follow-up calculations of the electrostatic contributions to the free energy of binding uncovered significantly stronger Coulombic interactions in complexes harbouring ID segments than in structured protein complexes. However, they are counter-balanced by even higher polar-desolvation penalties. We propose that polar interactions are a key contributing factor to the observed high specificity of ID segment-mediated interactions.
Highlights
In cells, communication is established principally by proteinprotein interactions [1]
In the light of the magnitude of the electrostatic energy terms that we estimated for intrinsically disordered (ID) complexes, we suggest that strong electrostatic interactions are a key component of the highly complementary interactions between ID segments and their partners that translates to high specificity
It has been shown that ID segments bury more solvent accessible surface area relative to their length than do structured proteins when they interact with other macromolecules [28]
Summary
Communication is established principally by proteinprotein interactions [1]. Specificity in interactions is believed to rely on shape complementarity, hydrogen bonding, and salt-bridge formation [13,14]. In this context, the role of electrostatics in proteinprotein interactions has been studied extensively [6,15]. It has been shown that salt bridges in protein interfaces can contribute favorably to protein stability and the free energy of binding through Coulombic interactions, but that this effect is often counterbalanced by very unfavorable desolvation [16,17,18,19,20,21]. This contribution is explained by the large energetic penalty for burying but not compensating for charged residues
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