| Literature DB >> 33067355 |
Elin Karlsson1, Cristina Paissoni2, Amanda M Erkelens3, Zeinab A Tehranizadeh3, Frieda A Sorgenfrei3, Eva Andersson3, Weihua Ye3, Carlo Camilloni2, Per Jemth3.
Abstract
Intrinsically disordered protein domains often have multiple binding partners. It is plausible that the strength of pairing with specific partners evolves from an initial low to higher affinity. However, little is known about the molecular changes in the binding mechanism that would facilitate such a transition. We previously showed that the interaction between two intrinsically disordered domains, NCBD and CID, likely emerged in an ancestral deuterostome organism as a low-affinity interaction that subsequently evolved into a higher-affinity interaction before the radiation of modern vertebrate groups. Here we map native contacts in the transition states of the low-affinity ancestral and high-affinity human NCBD/CID interactions. We show that the coupled binding and folding mechanism is overall similar, but with a higher degree of native hydrophobic contact formation in the transition state of the ancestral complex and more heterogeneous transient interactions, including electrostatic pairings, and an increased disorder for the human complex. Adaptation to new binding partners may be facilitated by this ability to exploit multiple alternative transient interactions while retaining the overall binding and folding pathway. Published under license by The American Society for Biochemistry and Molecular Biology, Inc.Keywords: IDP; Protein binding; coupled binding and folding; intrinsically disordered protein; pre-steady-state kinetics; protein complex; protein evolution; protein folding; transition state
Year: 2020 PMID: 33067355 DOI: 10.1074/jbc.RA120.015645
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157