The Role of Low Complexity Regions in Protein Interaction Modes: An Illustration in Huntingtin

6533b828fe1ef96bd1288f47

RESEARCH PRODUCT

The Role of Low Complexity Regions in Protein Interaction Modes: An Illustration in Huntingtin

Kristina Kastano Pablo Mier Miguel A. Andrade-navarro

subject

Protein Conformation alpha-Helical 0301 basic medicine Network complexity Huntingtin intrinsically disordered regions Amino Acid Motifs Computational biology Biology protein interactions Article compositionally biased regions Catalysis Protein–protein interaction lcsh:Chemistry Evolution Molecular Inorganic Chemistry Low complexity 03 medical and health sciences Protein Domains Protein Interaction Mapping Animals Humans p300-CBP Transcription Factors Amino Acid Sequence Protein Interaction Maps Huntingtin Tissue distribution Physical and Theoretical Chemistry lcsh:QH301-705.5 Molecular Biology Spectroscopy Huntingtin Protein 030102 biochemistry & molecular biology Organic Chemistry Nuclear Proteins p120 GTPase Activating Protein General Medicine Multiple modes Synapsins low complexity regions Computer Science Applications homorepeats Microscopy Electron 030104 developmental biology lcsh:Biology (General)lcsh:QD1-999 Sequence Alignment Function (biology)Protein Binding

description

Low complexity regions (LCRs) are very frequent in protein sequences, generally having a lower propensity to form structured domains and tending to be much less evolutionarily conserved than globular domains. Their higher abundance in eukaryotes and in species with more cellular types agrees with a growing number of reports on their function in protein interactions regulated by post-translational modifications. LCRs facilitate the increase of regulatory and network complexity required with the emergence of organisms with more complex tissue distribution and development. Although the low conservation and structural flexibility of LCRs complicate their study, evolutionary studies of proteins across species have been used to evaluate their significance and function. To investigate how to apply this evolutionary approach to the study of LCR function in protein–protein interactions, we performed a detailed analysis for Huntingtin (HTT), a large protein that is a hub for interaction with hundreds of proteins, has a variety of LCRs, and for which partial structural information (in complex with HAP40) is available. We hypothesize that proteins RASA1, SYN2, and KAT2B may compete with HAP40 for their attachment to the core of HTT using similar LCRs. Our results illustrate how evolution might favor the interplay of LCRs with domains, and the possibility of detecting multiple modes of LCR-mediated protein–protein interactions with a large hub such as HTT when enough protein interaction data is available.

year	journal	country	edition	language
2021-02-09	International Journal of Molecular Sciences

https://doi.org/10.3390/ijms22041727