Literature DB >> 25266743

Binding hotspots of BAZ2B bromodomain: Histone interaction revealed by solution NMR driven docking.

Fleur M Ferguson1, David M Dias, João P G L M Rodrigues, Hans Wienk, Rolf Boelens, Alexandre M J J Bonvin, Chris Abell, Alessio Ciulli.   

Abstract

Bromodomains are epigenetic reader domains, which have come under increasing scrutiny both from academic and pharmaceutical research groups. Effective targeting of the BAZ2B bromodomain by small molecule inhibitors has been recently reported, but no structural information is yet available on the interaction with its natural binding partner, acetylated histone H3K14ac. We have assigned the BAZ2B bromodomain and studied its interaction with H3K14ac acetylated peptides by NMR spectroscopy using both chemical shift perturbation (CSP) data and clean chemical exchange (CLEANEX-PM) NMR experiments. The latter was used to characterize water molecules known to play an important role in mediating interactions. Besides the anticipated Kac binding site, we consistently found the bromodomain BC loop as hotspots for the interaction. This information was used to create a data-driven model for the complex using HADDOCK. Our findings provide both structure and dynamics characterization that will be useful in the quest for potent and selective inhibitors to probe the function of the BAZ2B bromodomain.

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Year:  2014        PMID: 25266743      PMCID: PMC4458377          DOI: 10.1021/bi500909d

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  28 in total

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Authors:  Fleur M Ferguson; Oleg Fedorov; Apirat Chaikuad; Martin Philpott; Joao R C Muniz; Ildiko Felletar; Frank von Delft; Tom Heightman; Stefan Knapp; Chris Abell; Alessio Ciulli
Journal:  J Med Chem       Date:  2013-12-13       Impact factor: 7.446

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  11 in total

1.  Crystal structure of the BAZ2B TAM domain.

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2.  Dual Screening of BPTF and Brd4 Using Protein-Observed Fluorine NMR Uncovers New Bromodomain Probe Molecules.

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3.  Discovery of a hidden transient state in all bromodomain families.

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Review 10.  Small Molecules Targeting the Specific Domains of Histone-Mark Readers in Cancer Therapy.

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