Discovery, Synthesis, and Biological Evaluation of Orally Active Pyrrolidone Derivatives as Novel Inhibitors of p53–MDM2 Protein–Protein Interaction

Zhuang, Chunlin; Zhu, Lingjian; Dong, Guoqiang; Guo, Zizhao; Wang, Shengzheng; Zhang, Yongqiang; Wu, Yang‐Chang; Yao, Jing; Sheng, Chunquan; Zhang, Wannian

doi:10.1021/jm300969t

Cited by 116 publications

(105 citation statements)

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“…4 These small molecules have received much attention from academia and industry in the past decade, since the function of wild-type (WT) p53 is inactivated by overexpression 5 or amplification 6 of MDM2, even though the p53 gene is either deleted or mutated in approximately 50% of all human cancers. 7−9 Additionally, since MDM2 is overexpressed in many types of cancer and functions as a key negative regulator of wild-type p53, the Nutlins have shown promise as anticancer therapeutics. Hoffmann-La Roche (HLR) was the first to advance a Nutlin analogue (RG7112) into clinical trials for solid and hematological tumors.…”

Section: Introductionmentioning

confidence: 99%

Organocatalytic, Diastereo- and Enantioselective Synthesis of Nonsymmetric cis-Stilbene Diamines: A Platform for the Preparation of Single-Enantiomer cis-Imidazolines for Protein–Protein Inhibition

et al. 2014

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The finding by scientists at Hoffmann-La Roche that cis-imidazolines could disrupt the protein–protein interaction between p53 and MDM2, thereby inducing apoptosis in cancer cells, raised considerable interest in this scaffold over the past decade. Initial routes to these small molecules (i.e., Nutlin-3) provided only the racemic form, with enantiomers being enriched by chromatographic separation using high-pressure liquid chromatography (HPLC) and a chiral stationary phase. Reported here is the first application of an enantioselective aza-Henry approach to nonsymmetric cis-stilbene diamines and cis-imidazolines. Two novel mono(amidine) organocatalysts (MAM) were discovered to provide high levels of enantioselection (>95% ee) across a broad range of substrate combinations. Furthermore, the versatility of the aza-Henry strategy for preparing nonsymmetric cis-imidazolines is illustrated by a comparison of the roles of aryl nitromethane and aryl aldimine in the key step, which revealed unique substrate electronic effects providing direction for aza-Henry substrate–catalyst matching. This method was used to prepare highly substituted cis-4,5-diaryl imidazolines that project unique aromatic rings, and these were evaluated for MDM2-p53 inhibition in a fluorescence polarization assay. The diversification of access to cis-stilbene diamine-derived imidazolines provided by this platform should streamline their further development as chemical tools for disrupting protein–protein interactions.

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Section: Introductionmentioning

confidence: 99%

Organocatalytic, Diastereo- and Enantioselective Synthesis of Nonsymmetric cis-Stilbene Diamines: A Platform for the Preparation of Single-Enantiomer cis-Imidazolines for Protein–Protein Inhibition

et al. 2014

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“…RO-2443 forms two H-bonds with Gln72A, whereas NSC148171 only forms one H-bond with Gln72A. This may explain the difference in activity between RO-2443 (IC 50 ¼ 33 nM) 26 and NSC148171 (K i ¼ 620 nM) ( Fig. 5A and B).…”

Section: Insight Into the Binding Modes Of Active Compounds Against Mmentioning

confidence: 97%

“…While RO-2443 and RO-5963 share the same skeleton, K23, WW8, 4t and nutlin-3 possess similar pharmacophores. Second, several crystal structures of some of these compounds in complex with MDM2 and/or MDMX have been reported, 25,26 showing two different binding modes of MDM2/MDMX at the inhibitor-protein interface. MDM2 differs in binding mode between its complexes with RO-2443 (PDB CODE: 3VBG) and K23 (PDB CODE: 3LBK), whereas MDMX shows a difference in binding between its complexes with RO-2443 (PDB CODE: 3U15) and WW8 (PDB CODE: 3LBJ).…”

Section: Pharmacophore Model and Virtual Screeningmentioning

confidence: 99%

Rapid identification of dual p53-MDM2/MDMX interaction inhibitors through virtual screening and hit-based substructure search

Chen

Yuan

et al. 2017

RSC Adv.

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Multi-target agents have garnered great interest over the past decade for their favorable therapeutic efficacy and drug resistance profiles. Recently, dual inhibition of the p53 tumor suppressor interaction with its two negative regulators MDM2 and MDMX has become an attractive anticancer approach as it can induce sustained MDM2/MDMX antagonism and robust p53 activation. However, small molecule inhibitors with dual specificity against MDM2 and MDMX are difficult to design and are still scarce. To identify novel scaffolds for dual inhibition of the p53-MDM2/MDMX interactions, we developed two fivepoint pharmacophore models for filtering the 2012 National Cancer Institute database, from which molecular docking was conducted to identify dual inhibitors. We found 38 virtual hits and subjected them to a fluorescence polarization-based competitive binding assay, resulting in 10 active compounds of different scaffolds. To further expand the chemical diversity of the initial hits, we performed a hitbased substructure search and identified NSC148171 from pharmacophore 1 as the most potent dualspecificity inhibitor with K i values for MDM2 and MDMX at 0.62 and 4.6 mM. All hits were subjected to inhibition assay of cancer cellular vitality and showed anti-proliferative activity roughly correlated with their K i values. This work not only yields several novel scaffolds for further structural and functional optimization of dual-specificity inhibitors of the p53-MDM2/MDMX interactions, but also showcases the power of our computational methods for small molecule anticancer drug discovery.

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“…Structure-based design has also led to the development of several other molecules that target MDM2's hydrophobic cleft using various chemical scaffolds, such as methylbenzo-amines (Dudgeon et al, 2010), imidazole-indoles (Czarna et al, 2010), isoindolinones (Hardcastle et al, 2006; Hardcastle et al, 2011; Riedinger et al, 2011), pyrrolopyrimidines (Lee et al, 2011), sulphonamides (Galatin & Abraham, 2004), and benzodiazepines (Z. Yu et al, 2014; Zhuang et al, 2011), which all demonstrate nanomolar binding affinities to MDM2 and with one pyrrolidinone exhibiting dual MDM2/MDMX activity (Zhuang et al, 2012) and one pyrrolopyrazole seemingly active against both MDM2 and the NF-κB complex (Zhuang et al, 2014), a different cancer-related pathway (DiDonato, Mercurio, & Karin, 2012). Perhaps most promising are a series of piperidonones (AM-8553, AM-7209, AMG 232) and morpholinones (AM-8735) developed from Amgen laboratories that exhibit exceptional pharmacokinetic properties, such as low clearance rate, long half-life, and high oral bioavailability (Gonzalez-Lopez de Turiso et al, 2013; Gonzalez, Eksterowicz, et al, 2014; Rew et al, 2012; Rew et al, 2014; Sun et al, 2014).…”

Section: Small Molecule Wild-type P53 Activatorsmentioning

confidence: 99%

Reviving the guardian of the genome: Small molecule activators of p53

Nguyen

Liao

Zeng

et al. 2017

Pharmacology & Therapeutics

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The tumor suppressor p53 is one of the most important proteins for protection of genomic stability and cancer prevention. Cancers often inactivate it by either mutating its gene or disabling its function. Thus, activating p53 becomes an attractive approach for the development of molecule-based anti-cancer therapy. The past decade and half have witnessed tremendous progress in this area. This essay offers readers with a grand review on this progress with updated information about small molecule activators of p53 either still at bench work or in clinical trials.

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Discovery, Synthesis, and Biological Evaluation of Orally Active Pyrrolidone Derivatives as Novel Inhibitors of p53–MDM2 Protein–Protein Interaction

Cited by 116 publications

References 50 publications

Organocatalytic, Diastereo- and Enantioselective Synthesis of Nonsymmetric cis-Stilbene Diamines: A Platform for the Preparation of Single-Enantiomer cis-Imidazolines for Protein–Protein Inhibition

Organocatalytic, Diastereo- and Enantioselective Synthesis of Nonsymmetric cis-Stilbene Diamines: A Platform for the Preparation of Single-Enantiomer cis-Imidazolines for Protein–Protein Inhibition

Rapid identification of dual p53-MDM2/MDMX interaction inhibitors through virtual screening and hit-based substructure search

Reviving the guardian of the genome: Small molecule activators of p53

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