Observed bromodomain flexibility reveals histone peptide- and small molecule ligand-compatible forms of ATAD2

Poncet-Montange, G.; Zhan, Yanai; Bardenhagen, Jennifer; Petrocchi, Alessia; Leo, Elisabetta; Shi, Xi; Lee, Gilbert R.; Leonard, Paul G.; Geck, Mary; Cardozo, Mario; Andersen, Jannik N.; Palmer, Wylie S.; Jones, Philip; Ladbury, John E.

doi:10.1042/bj20140933

Cited by 34 publications

(104 citation statements)

References 46 publications

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“…56 Despite this, the resulting dimethyl isoxazole hit 59 had Kd for ATAD2 of 200 μM (LE 0.28), comparable to that reported for the similar isoxazole fragments 7 and 14 to the BET bromodomain (see above) It also found that known inhibitors of other bromodomains were relatively weak against ATAD2.…”

Section: Atad2 and Water Network-displacing Fragmentssupporting

confidence: 64%

“…Some fragments bind to ATAD2 and other bromodomains with unexpected displacement of some or all of the waters of the conserved network. 56 The optimisation of selective CREBBP inhibitors was assisted by a pocket created by the movement of a flexible arginine sidechain, which was not visible in the unbound crystal structure (Fig. In addition, the KAc-site environment is formed by the ZA and BC loop regions between α-helices, which have been seen to be mobile by solution NMR spectroscopy.…”

Section: Resultsmentioning

confidence: 99%

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Fragments in bromodomain drug discovery

Bamborough

Chung

2015

Med. Chem. Commun.

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Fragment-based approaches have been successfully applied to the discovery and optimisation of ligands for a wide range of targets. These concepts are proving valuable for bromodomain-containing proteins, an emerging family of epigenetic regulators. This review gives examples in which fragment-based drug discovery concepts are helping to find and optimise bromodomain inhibitors, with early successes against the BET subfamily now extending to other members of the target class.Med. Chem. Commun. This journal is

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Section: Atad2 and Water Network-displacing Fragmentssupporting

confidence: 64%

Section: Resultsmentioning

confidence: 99%

Fragments in bromodomain drug discovery

Bamborough

Chung

2015

Med. Chem. Commun.

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“…Equally encouraging are inhibitors that have now been identified for more difficult to drug bromodomains, 18 such as BAZ2B 19, 20 and ATAD2A. 21-23 Unlike the BET sub-family, which contain two bromodomains that primarily drive their binding and therefore function, a large proportion of the other BCPs contain auxiliary domains, many with diverse and sometimes unknown functions. These multi-domain containing BCPs can also be part of multi-protein complexes.…”

Section: Introductionmentioning

confidence: 99%

Structure-Guided Design of IACS-9571, a Selective High-Affinity Dual TRIM24-BRPF1 Bromodomain Inhibitor

et al. 2015

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The bromodomain containing proteins TRIM24 (Tripartite motif containing protein 24) and BRPF1 (bromodomain and PHD finger containing protein 1) are involved in the epigenetic regulation of gene expression and have been implicated in human cancer. Overexpression of TRIM24 correlates with poor patient prognosis and BRPF1 is a scaffolding protein required for the assembly of histone acetyltransferase complexes, where the gene of MOZ (monocytic leukemia zinc finger protein) was first identified as a recurrent fusion partner in leukemia patients (8p11 chromosomal rearrangements). Here, we present the structure guided development of a series of N,N-dimethyl benzimidazolone bromodomain inhibitors through the iterative use of X-ray cocrystal structures. A unique binding mode enabled the design of a potent and selective inhibitor, 8i (IACS-9571) with low nanomolar affinities for TRIM24 and BRPF1 (ITC Kd = 31 nM and 14 nM, respectively). With its excellent cellular potency (EC50 = 50 nM) and favorable pharmacokinetic properties (F = 29%), 8i is a high-quality chemical probe for the evaluation of TRIM24 and/or BRPF1 bromodomain function in vitro and in vivo.

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“…15 One such bromodomain-containing protein is the ATPase family, AAA domain-containing protein 2 (ATAD2, UniProtKB Q6PL18, also called ANCCA/PRO 2000). 16 ATAD2 has been shown to recognize histone H4 that is acetylated at lysine 5 (H4K5ac) and lysine 12 (H4K12ac), 17,18 and has recently been proposed to function as a reader of newly synthesized H4K5acK12ac di-acetyllysine marks during DNA replication. 19 Several studies suggest a role for ATAD2 in the pathogenesis of cancer where it functions as a co-regulator of oncogenic transcription factors including E2F, 20,21 the estrogen receptorα, 16 the androgen receptor 22 , and MYC.…”

mentioning

confidence: 99%

“…25,26,30,35,43 This pattern across multiple cancers makes the ATAD2 bromodomain an attractive target for cancer therapy, and several inhibitors are currently in development. 17,[47][48][49][50] To further investigate structural features of the ATAD2 bromodomain that contribute to histone ligand and small molecule inhibitor Invitrogen) cells (ATAD2 CO). An ATAD2 bromodomain C1101A mutant protein was created using site-directed mutagenesis with the QuikChange II kit (Agilent).…”

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confidence: 99%

Disulfide bridge formation influences ligand recognition by the ATAD2 bromodomain

et al. 2018

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The ATPase family, AAA domain-containing protein 2 (ATAD2) has a C-terminal bromodomain, which functions as a chromatin reader domain recognizing acetylated lysine on the histone tails within the nucleosome. ATAD2 is overexpressed in many cancers and its expression is correlated with poor patient outcomes, making it an attractive therapeutic target and potential biomarker. We solved the crystal structure of the ATAD2 bromodomain and found that it contains a disulfide bridge near the base of the acetyllysine binding pocket (Cys1057-Cys1079). Sitedirected mutagenesis revealed that removal of a free C-terminal cysteine (C1101) residue greatly improved the solubility of the ATAD2 bromodomain in vitro. Isothermal titration calorimetry experiments in combination with the Ellman's assay demonstrated that formation of an intramolecular disulfide bridge negatively impacts the ligand binding affinities and alters the thermodynamic parameters of the ATAD2 bromodomain interaction with a histone H4K5ac peptide as well as a small molecule bromodomain ligand. Molecular dynamics simulations indicate that the formation of the disulfide bridge in the ATAD2 bromodomain does not alter the structure of the folded state or flexibility of the acetyllysine binding pocket. However, consideration of this unique structural feature should be taken into account when examining ligandbinding affinity, or in the design of new bromodomain inhibitor compounds that interact with this acetyllysine reader module. K E Y W O R D S acetyllysine, ATAD2, bromodomain inhibitor, chromatin reader domain, disulfide bridge, epigenetics, histone, post-translational modification

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Observed bromodomain flexibility reveals histone peptide- and small molecule ligand-compatible forms of ATAD2

Cited by 34 publications

References 46 publications

Fragments in bromodomain drug discovery

Fragments in bromodomain drug discovery

Structure-Guided Design of IACS-9571, a Selective High-Affinity Dual TRIM24-BRPF1 Bromodomain Inhibitor

Disulfide bridge formation influences ligand recognition by the ATAD2 bromodomain

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