Engagement of intrinsic disordered proteins in protein-protein interaction

Irena Roterman; Katarzyna Stapor; Leszek Konieczny

doi:10.3389/fmolb.2023.1230922

Engagement of intrinsic disordered proteins in protein-protein interaction

Front Mol Biosci. 2023 Jul 31:10:1230922. doi: 10.3389/fmolb.2023.1230922. eCollection 2023.

Authors

Irena Roterman¹, Katarzyna Stapor², Leszek Konieczny³

Affiliations

¹ Department of Bioinformatics and Telemedicine, Jagiellonian University-Medical College, Kraków, Poland.
² Department of Applied Informatics, Faculty of Automatic, Electronics and Computer Science, Silesian University of Technology, Gliwice, Poland.
³ Chair of Medical Biochemistry, Medical College, Jagiellonian University, Kraków, Poland.

Abstract

Proteins from the intrinsically disordered group (IDP) focus the attention of many researchers engaged in protein structure analysis. The main criteria used in their identification are lack of secondary structure and significant structural variability. This variability takes forms that cannot be identified in the X-ray technique. In the present study, different criteria were used to assess the status of IDP proteins and their fragments recognized as intrinsically disordered regions (IDRs). The status of the hydrophobic core in proteins identified as IDPs and in their complexes was assessed. The status of IDRs as components of the ordering structure resulting from the construction of the hydrophobic core was also assessed. The hydrophobic core is understood as a structure encompassing the entire molecule in the form of a centrally located high concentration of hydrophobicity and a shell with a gradually decreasing level of hydrophobicity until it reaches a level close to zero on the protein surface. It is a model assuming that the protein folding process follows a micellization pattern aiming at exposing polar residues on the surface, with the simultaneous isolation of hydrophobic amino acids from the polar aquatic environment. The use of the model of hydrophobicity distribution in proteins in the form of the 3D Gaussian distribution described on the protein particle introduces the possibility of assessing the degree of similarity to the assumed micelle-like distribution and also enables the identification of deviations and mismatch between the actual distribution and the idealized distribution. The FOD (fuzzy oil drop) model and its modified FOD-M version allow for the quantitative assessment of these differences and the assessment of the relationship of these areas to the protein function. In the present work, the sections of IDRs in protein complexes classified as IDPs are analyzed. The classification "disordered" in the structural sense (lack of secondary structure or high flexibility) does not always entail a mismatch with the structure of the hydrophobic core. Particularly, the interface area, often consisting of IDRs, in many analyzed complexes shows the compliance of the hydrophobicity distribution with the idealized distribution, which proves that matching to the structure of the hydrophobic core does not require secondary structure ordering.

Keywords: MoRF IR; disport; function-related structural changes; hydrophobicity; intrinsically disordered proteins; order-to-disorder; protein complex.

Grants and funding

This research was funded by Jagiellonian University Medical College, grant number N41/DBS/000722. This research was partially supported by the European Union’s Horizon 2020 Program under grant no. 857533 and the Sano project carried out within the International Research Agendas Program of the Foundation for Polish Science and was co-financed by the European Union under the European Regional Development Fund.