Literature DB >> 33592170

A common binding motif in the ET domain of BRD3 forms polymorphic structural interfaces with host and viral proteins.

Sriram Aiyer1, G V T Swapna1, Li-Chung Ma1, Gaohua Liu2, Jingzhou Hao3, Gordon Chalmers4, Brian C Jacobs5, Gaetano T Montelione6, Monica J Roth7.   

Abstract

The extraterminal (ET) domain of BRD3 is conserved among BET proteins (BRD2, BRD3, BRD4), interacting with multiple host and viral protein-protein networks. Solution NMR structures of complexes formed between the BRD3 ET domain and either the 79-residue murine leukemia virus integrase (IN) C-terminal domain (IN329-408) or its 22-residue IN tail peptide (IN386-407) alone reveal similar intermolecular three-stranded β-sheet formations. 15N relaxation studies reveal a 10-residue linker region (IN379-388) tethering the SH3 domain (IN329-378) to the ET-binding motif (IN389-405):ET complex. This linker has restricted flexibility, affecting its potential range of orientations in the IN:nucleosome complex. The complex of the ET-binding peptide of the host NSD3 protein (NSD3148-184) and the BRD3 ET domain includes a similar three-stranded β-sheet interaction, but the orientation of the β hairpin is flipped compared with the two IN:ET complexes. These studies expand our understanding of molecular recognition polymorphism in complexes of ET-binding motifs with viral and host proteins.
Copyright © 2021 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  BET proteins; BRD3; Moloney murine leukemia virus; NSD3; extraterminal domain; integrase; interdomain dynamics; isotope peptide labeling; solution NMR

Mesh:

Substances:

Year:  2021        PMID: 33592170      PMCID: PMC8349776          DOI: 10.1016/j.str.2021.01.010

Source DB:  PubMed          Journal:  Structure        ISSN: 0969-2126            Impact factor:   5.006


  68 in total

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