| Literature DB >> 31178221 |
Tiago N Cordeiro1, Nathalie Sibille2, Pierre Germain2, Philippe Barthe2, Abdelhay Boulahtouf3, Fréderic Allemand2, Rémy Bailly2, Valérie Vivat4, Christine Ebel5, Alessandro Barducci2, William Bourguet2, Albane le Maire6, Pau Bernadó7.
Abstract
In its unliganded form, the retinoic acid receptor (RAR) in heterodimer with the retinoid X receptor (RXR) exerts a strong repressive activity facilitated by the recruitment of transcriptional corepressors in the promoter region of target genes. By integrating complementary structural, biophysical, and computational information, we demonstrate that intrinsic disorder is a required feature for the precise regulation of RAR activity. We show that structural dynamics of RAR and RXR H12 regions is an essential mechanism for RAR regulation. Unexpectedly we found that, while mainly disordered, the corepressor N-CoR presents evolutionary conserved structured regions involved in transient intramolecular contacts. In the presence of RXR/RAR, N-CoR exploits its multivalency to form a cooperative multisite complex that displays equilibrium between different conformational states that can be tuned by cognate ligands and receptor mutations. This equilibrium is key to preserving the repressive basal state while allowing the conversion to a transcriptionally active form.Entities:
Keywords: Nuclear Magnetic Resonance; corepressor; dynamic protein complex; integrative structural biology; intrinsically disordered protein; multivalent protein; retinoic acid receptor; small-angle X-ray scattering; structural modeling; transcriptional regulation
Mesh:
Substances:
Year: 2019 PMID: 31178221 DOI: 10.1016/j.str.2019.05.001
Source DB: PubMed Journal: Structure ISSN: 0969-2126 Impact factor: 5.006