Small-molecule inhibition of MLL activity by disruption of its interaction with WDR5

Senisterra, Guillermo; Wu, Hong; Allali-Hassani, Abdellah; Wasney, Gregory A.; Baršytė-Lovejoy, Dalia; Dombrovski, L.; Dong, Aiping; Nguyen, Kong T.; Smil, D.; Bolshan, Yuri; Hajian, Taraneh; He, Hao; Seitova, A.; Chau, Irene; Li, Fengling; Poda, Gennadiy; Couture, Jean-François; Brown, Peter J.; Al‐awar, Rima; Schapira, Matthieu; Arrowsmith, C.H.; Vedadi, Masoud

doi:10.1042/bj20121280

Cited by 135 publications

(131 citation statements)

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“…23 In this assay, binding of the fluorescein-labeled peptide to WDR5 (K D = 458 ± 45 nM) increases the FP signal. Binding compounds compete with and displace the labeled peptide, resulting in the reduction of signal.…”

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confidence: 92%

“…As expected, the compound occupies the central cavity of WDR5 and recapitulates interactions previously observed with less potent analogs (PDB codes 3SMR and 3UR4), including direct and water mediated hydrogen bonds with S91 and C261, opening-up of a cavity occupied by the nitro group, and aromatic stacking with F133. 23 The conformation of side chains within 4 Å of the compound is almost perfectly conserved (RMSD = 0.15 Å). The scaffold sits in the pocket, adopting a conformation closer to that observed for the 2-chlorophenyl analog (RMSD = 0.33 Å, PDB code 3SMR) versus that of the 3-methoxyphenyl analog (RMSD = 1.47 Å, PDB code 3UR4).…”

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confidence: 97%

“…25 As part of our ongoing research involving the discovery and development of potent, selective, and cell-permeable small molecule inhibitors (chemical probes) for epigenetic proteins, 26 we recently disclosed several novel compounds that antagonize WDR5−MLL interaction, including WDR5-0102 (2) ( Figure 1). 23 This proof of principle study prompted us to undertake the SAR-driven optimization of prototypic antagonist WDR5-0102 (2) described in this Letter, leading eventually to preparation of the more potent antagonist 47.…”

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confidence: 99%

“…11,12,23 The amide group of 2 forms one direct and one water-mediated (W517) hydrogen bond with the side chain of S91 and the backbone nitrogen of C261, respectively. The N-methylpiperazine moiety, predicted to be significantly protonated at physiological pH, 27 forms a water-mediated (W576) hydrogen bond with the backbone carbonyl of C261, and it occupies the bottom of the pocket.…”

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confidence: 99%

“…23 To better understand the increased potency of compound 47, we solved its structure in complex with WDR5 (PDB code 4IA9) ( Figure 3). As expected, the compound occupies the central cavity of WDR5 and recapitulates interactions previously observed with less potent analogs (PDB codes 3SMR and 3UR4), including direct and water mediated hydrogen bonds with S91 and C261, opening-up of a cavity occupied by the nitro group, and aromatic stacking with F133.…”

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confidence: 99%

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Synthesis, Optimization, and Evaluation of Novel Small Molecules as Antagonists of WDR5-MLL Interaction

Bolshan

Getlik

Kuznetsova

et al. 2013

ACS Med. Chem. Lett.

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The WD40-repeat protein WDR5 plays a critical role in maintaining the integrity of MLL complexes and fully activating their methyltransferase function. MLL complexes, the trithorax-like family of SET1 methyltransferases, catalyze trimethylation of lysine 4 on histone 3, and they have been widely implicated in various cancers. Antagonism of WDR5 and MLL subunit interaction by small molecules has recently been presented as a practical way to inhibit activity of the MLL1 complex, and N-(2-(4-methylpiperazin-1-yl)-5-substituted-phenyl) benzamides were reported as potent and selective antagonists of such an interaction. Here, we describe the protein crystal structure guided optimization of prototypic compound 2 (K dis = 7 μM), leading to identification of more potent antagonist 47 (K dis = 0.3 μM). KEYWORDS: WDR5, MLL, SET1 methyltransferase complex, peptide binding site, small molecule antagonists T he SET1-family of human histone methyltransferases (SET1A, SET1B, MLL1, MLL2, MLL3, and MLL4) contribute to active chromatin via mono-, di-, and trimethylation of lysine 4 on histone H3. 1−3 MLLs are S-adenosyl methionine (SAM) dependent lysine methyltransferases that work optimally when in complex with other components; WDR5 (WD40 repeat protein 5), RbBP5 (retinoblastomabinding protein-5), ASH2L (absent small homeotic disks-2-like), and DPY-30 (WRAD). 4 WDR5 has been shown to be essential for complex integrity and for fully activating MLL methyltransferase function. 5−7 In the peptide-bound structure, WDR5 adopts a donutshaped WD40-repeat fold with a deep central cavity that normally accommodates an arginine side chain of interacting peptides. 8 WDR5 binds to the "WDR5 INteracting" (WIN) motif of MLL1 through the peptidyl arginine-binding cleft. 8−12 A crystal structure of WDR5 in complex with MLL1 WIN peptide revealed the critical role of arginine 3765 of MLL1 in complex formation. 9 A similar interaction has been reported for WDR5 and the WIN region of all SET1 family lysine methyltransferases, with reported K D values of 1.13, 0.16, 2.03, 0.03, 0.26, and 0.10 μM for MLL1-4, SET1A, and SET1B WIN peptides, respectively. 13 Although there is significant divergence in the amino acid sequences of WIN motifs close to the critical arginine residue, the plasticity of the WDR5 arginine binding pocket allows such an interaction with the WIN motifs of all MLLs. 13 MLLs have been reported to be essential for embryonic development and biological processes 14−17 and have been widely implicated in a variety of cancers. 18−22 As almost all MLLs show minimal or no activity in the absence of the complex components (WDR5 in particular), 13 identifying WDR5−MLL interaction antagonists has been proposed as a potentially selective alternative to active site directed inhibitors of MLL methyltransferase activity. Such antagonists could serve as a starting point for the development of potential therapeutics to treat MLL-rearranged leukemias or other related cancers. 23 Recent reports detailing the use of short arginine contain...

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confidence: 92%

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