Literature DB >> 24333487

Molecular insights into the recognition of N-terminal histone modifications by the BRPF1 bromodomain.

Amanda Poplawski1, Kaifeng Hu2, Woonghee Lee2, Senthil Natesan1, Danni Peng3, Samuel Carlson1, Xiaobing Shi3, Stefan Balaz1, John L Markley2, Karen C Glass4.   

Abstract

The monocytic leukemic zinc finger (MOZ) histone acetyltransferase (HAT) acetylates free histones H3, H4, H2A, and H2B in vitro and is associated with up-regulation of gene transcription. The MOZ HAT functions as a quaternary complex with the bromodomain-PHD finger protein 1 (BRPF1), inhibitor of growth 5 (ING5), and hEaf6 subunits. BRPF1 links the MOZ catalytic subunit to the ING5 and hEaf6 subunits, thereby promoting MOZ HAT activity. Human BRPF1 contains multiple effector domains with known roles in gene transcription, as well as chromatin binding and remodeling. However, the biological function of the BRPF1 bromodomain remains unknown. Our findings reveal novel interactions of the BRPF1 bromodomain with multiple acetyllysine residues on the N-terminus of histones and show that it preferentially selects for H2AK5ac, H4K12ac, and H3K14ac. We used chemical shift perturbation data from NMR titration experiments to map the BRPF1 bromodomain ligand binding pocket and identified key residues responsible for coordination of the post-translationally modified histones. Extensive molecular dynamics simulations were used to generate structural models of bromodomain-histone ligand complexes, to analyze hydrogen bonding and other interactions, and to calculate the binding free energies. Our results outline the molecular mechanism driving binding specificity of the BRPF1 bromodomain for discrete acetyllysine residues on the N-terminal histone tails. Together, these data provide insights into how histone recognition by the bromodomain directs the biological function of BRPF1, ultimately targeting the MOZ HAT complex to chromatin substrates.
Copyright © 2013 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  bromodomain; epigenetics; histone acetyltransferase; molecular dynamic simulations; nuclear magnetic resonance

Mesh:

Substances:

Year:  2013        PMID: 24333487      PMCID: PMC3969779          DOI: 10.1016/j.jmb.2013.12.007

Source DB:  PubMed          Journal:  J Mol Biol        ISSN: 0022-2836            Impact factor:   5.469


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