Abstract
Intrinsically disordered proteins (IDPs) exist without the presence of a stable tertiary structure in isolation. These proteins are often involved in molecular recognition processes via their disordered binding regions that can recognize partner molecules by undergoing a coupled folding and binding process. The specific properties of disordered binding regions give way to specific, yet transient interactions that enable IDPs to play central roles in signaling pathways and act as hubs of protein interaction networks. An alternative model of protein-protein interactions with largely overlapping functional properties is offered by the concept of linear interaction motifs. This approach focuses on distilling a short consensus sequence pattern from proteins with a common interaction partner. These motifs often reside in disordered regions and are considered to mediate the interaction roughly independent from the rest of the protein. Although a connection between linear motifs and disordered binding regions has been established through common examples, the complementary nature of the two concepts has yet to be fully explored. In many cases the sequence based definition of linear motifs and the structural context based definition of disordered binding regions describe two aspects of the same phenomenon. To gain insight into the connection between the two models, prediction methods were utilized. We combined the regular expression based prediction of linear motifs with the disordered binding region prediction method ANCHOR, each specialized for either model to get the best of both worlds. The thorough analysis of the overlap of the two methods offers a bioinformatics tool for more efficient binding site prediction that can serve a wide range of practical implications. At the same time it can also shed light on the theoretical connection between the two co-existing interaction models.
Highlights
Most proteins carry out their function through recognizing and binding to partner molecules, a vast majority of which are proteins themselves
Predictive Power of Linear Motifs One of the main limitations of using linear motifs in the prediction of protein-protein binding regions is the weak definition of the motifs
The two major frameworks in which these interactions are studied are the concepts of linear motifs and disordered binding regions
Summary
Most proteins carry out their function through recognizing and binding to partner molecules, a vast majority of which are proteins themselves. Studying the details of this molecular recognition process is essential to understand the organization of living cells [1]. Following the appearance of the first protein structures the dominant view of protein-protein interactions was represented by interactions between well-folded domains, where two protein domains interact as a result of steric, hydrophobic and charge complementarity of their interacting surfaces [2]. Later it was recognized that a large fraction of protein-protein interactions are not mediated exclusively by folded domains. Interactions involving non-folded domains represent a distinct type of binding mode that is prevalent in various regulatory and signaling processes [3–6]. In this work we study the relationship between two related concepts that were introduced to describe such interactions: disordered binding regions and linear interaction motifs
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