Your search keyword '"Emmanuel Hubert Demont"' showing total 40 results

1. Discovery of a Highly Selective BET BD2 Inhibitor from a DNA-Encoded Library Technology Screening Hit

Author

Stephen John Atkinson, Patricia F Medeiros, Paola Grandi, Simon Taylor, Chun-wa Chung, James Gray, Robert J. Watson, Ian D. Wall, Alexander L. Satz, Rab K. Prinjha, Francesco Rianjongdee, Alex Preston, Emmanuel Hubert Demont, Gang Yao, Alex Phillipou, Inmaculada Rioja, Cassie Messenger, and Laura J. Kaushansky

Subjects

Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Drug Evaluation, Preclinical, Proteins, chemical and pharmacologic phenomena, hemic and immune systems, Chemical probe, Clinical settings, DNA, Computational biology, Highly selective, Bromodomain, Small Molecule Libraries, Structure-Activity Relationship, Safety profile, Protein Domains, Drug Discovery, Humans, Molecular Medicine, A-DNA

Abstract

Second-generation bromodomain and extra terminal (BET) inhibitors, which selectively target one of the two bromodomains in the BET proteins, have begun to emerge in the literature. These inhibitors aim to help determine the roles and functions of each domain and assess whether they can demonstrate an improved safety profile in clinical settings compared to pan-BET inhibitors. Herein, we describe the discovery of a novel BET BD2-selective chemotype using a structure-based drug design from a hit identified by DNA-encoded library technologies, showing a structural differentiation from key previously reported greater than 100-fold BD2-selective chemotypes GSK620, GSK046, and ABBV-744. Following a structure-based hypothesis for the selectivity and optimization of the physicochemical properties of the series, we identified 60 (GSK040), an in vitro ready and in vivo capable BET BD2-inhibitor of unprecedented selectivity (5000-fold) against BET BD1, excellent selectivity against other bromodomains, and good physicochemical properties. This novel chemical probe can be added to the toolbox used in the advancement of epigenetics research.

Published

2021

2. Identification of a Series of N-Methylpyridine-2-carboxamides as Potent and Selective Inhibitors of the Second Bromodomain (BD2) of the Bromo and Extra Terminal Domain (BET) Proteins

Author

Antonia J. Lewis, Anna K. Bassil, Lee Andrew Harrison, Darren Jason Mitchell, Dave Lugo, Robert J. Watson, James Gray, Rab K. Prinjha, Alex Preston, Anne-Marie Michon, Ian D. Wall, Simon Taylor, Chun-wa Chung, Jonathan Thomas Seal, Stephen John Atkinson, Etienne Levernier, Paola Grandi, Emmanuel Hubert Demont, Inmaculada Rioja, James Michael Woolven, and Cassie Messenger

Subjects

BRD4, Drug discovery, Chemistry, In vivo, Drug Discovery, Aqueous solubility, Molecular Medicine, Molecule, Solubility, Selectivity, Combinatorial chemistry, Bromodomain

Abstract

Domain-specific BET bromodomain ligands represent an attractive target for drug discovery with the potential to unlock the therapeutic benefits of antagonizing these proteins without eliciting the toxicological aspects seen with pan-BET inhibitors. While we have reported several distinct classes of BD2 selective compounds, namely, GSK620, GSK549, and GSK046, only GSK046 shows high aqueous solubility. Herein, we describe the lead optimization of a further class of highly soluble compounds based upon a picolinamide chemotype. Focusing on achieving >1000-fold selectivity for BD2 over BD1 ,while retaining favorable physical chemical properties, compound 36 was identified as being 2000-fold selective for BD2 over BD1 (Brd4 data) with >1 mg/mL solubility in FaSSIF media. 36 represents a valuable new in vivo ready molecule for the exploration of the BD2 phenotype.

Published

2021

3. Template-Hopping Approach Leads to Potent, Selective, and Highly Soluble Bromo and Extraterminal Domain (BET) Second Bromodomain (BD2) Inhibitors

Author

Emmanuel Hubert Demont, Jonathan Thomas Seal, Stephen John Atkinson, Anna K. Bassil, Paola Grandi, Robert J. Watson, Thomas George Christopher Hayhow, James Gray, Chun-wa Chung, Aylott Helen Elizabeth, Alexander N Phillipou, Darren Jason Mitchell, James Michael Woolven, Inmaculada Rioja, Laurie J. Gordon, Francesco Rianjongdee, Paul Bamborough, Ian D. Wall, Rab K. Prinjha, Alex Preston, Lee Andrew Harrison, and Cassie Messenger

Subjects

0303 health sciences, Drug discovery, Cell Cycle Proteins, 01 natural sciences, Combinatorial chemistry, 0104 chemical sciences, Bromodomain, Small Molecule Libraries, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, chemistry.chemical_compound, Protein Domains, chemistry, Drug Design, Amide, Drug Discovery, Humans, Molecular Medicine, Acetamide, Transcription Factors, 030304 developmental biology

Abstract

A number of reports have recently been published describing the discovery and optimization of bromo and extraterminal inhibitors which are selective for the second bromodomain (BD2); these include our own work toward GSK046 (3) and GSK620 (5). This paper describes our approach to mitigating the genotoxicity risk of GSK046 by replacement of the acetamide functionality with a heterocyclic ring. This was followed by a template-hopping and hybridization approach, guided by structure-based drug design, to incorporate learnings from other BD2-selective series, optimize the vector for the amide region, and explore the ZA cleft, leading to the identification of potent, selective, and bioavailable compounds 28 (GSK452), 39 (GSK737), and 36 (GSK217).

Published

2021

4. The Optimization of a Novel, Weak Bromo and Extra Terminal Domain (BET) Bromodomain Fragment Ligand to a Potent and Selective Second Bromodomain (BD2) Inhibitor

Author

Stephen John Atkinson, Royston C. B. Copley, Matthew J Lindon, Rab K. Prinjha, Alex Preston, James Michael Woolven, Jonathan Thomas Seal, Chun-wa Chung, James Gray, Thomas George Christopher Hayhow, Laurie J. Gordon, Emmanuel Hubert Demont, Aylott Helen Elizabeth, Paola Grandi, Lee Andrew Harrison, Inmaculada Rioja, Robert J. Watson, Simon Taylor, Cassie Messenger, Ian D. Wall, Anne-Marie Michon, Darren Jason Mitchell, and Paul Bamborough

Subjects

Male, Stereochemistry, Protein domain, Anti-Inflammatory Agents, Administration, Oral, Cell Cycle Proteins, Molecular Dynamics Simulation, Crystallography, X-Ray, Ligands, Structure-Activity Relationship, Dogs, Protein Domains, In vivo, Drug Discovery, Animals, Humans, Structure–activity relationship, Rats, Wistar, Binding site, Binding Sites, Chemistry, Ligand, Hydrogen Bonding, Amides, Phenotype, Rats, Bromodomain, Molecular Medicine, Selectivity, Half-Life, Transcription Factors

Abstract

The profound efficacy, yet associated toxicity of pan-BET inhibitors is well documented. The possibility of an ameliorated safety profile driven by significantly selective (>100-fold) inhibition of a subset of the eight bromodomains is enticing, but challenging given the close homology. Herein, we describe the X-ray crystal structure-directed optimization of a novel weak fragment ligand with a pan-second bromodomain (BD2) bias, to potent and highly BD2 selective inhibitors. A template hopping approach, enabled by our parallel research into an orthogonal template (15, GSK046), was the basis for the high selectivity observed. This culminated in two tool molecules, 20 (GSK620) and 56 (GSK549), which showed an anti-inflammatory phenotype in human whole blood, confirming their cellular target engagement. Excellent broad selectivity, developability, and in vivo oral pharmacokinetics characterize these tools, which we hope will be of broad utility to the field of epigenetics research.

Published

2020

5. Design and Synthesis of a Highly Selective and In Vivo-Capable Inhibitor of the Second Bromodomain of the Bromodomain and Extra Terminal Domain Family of Proteins

Author

Peter D. Craggs, Darren Jason Mitchell, Rab K. Prinjha, Alex Preston, James Michael Woolven, Laurie J. Gordon, Simon Taylor, Paul Bamborough, Chun-wa Chung, Paola Grandi, James Gray, Francesco Rianjongdee, Matthew J Lindon, Anne-Marie Michon, Emma J. Jones, Inmaculada Rioja, Robert J. Watson, Ian D. Wall, Stephen John Atkinson, Emmanuel Hubert Demont, and Jonathan Thomas Seal

Subjects

0303 health sciences, Chemistry, Protein domain, Highly selective, 01 natural sciences, Phenotype, In vitro, 0104 chemical sciences, Cell biology, Bromodomain, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, In vivo, Drug Discovery, Molecular Medicine, Structure–activity relationship, Binding site, 030304 developmental biology

Abstract

Pan-bromodomain and extra terminal domain (BET) inhibitors interact equipotently with the eight bromodomains of the BET family of proteins and have shown profound efficacy in a number of in vitro phenotypic assays and in vivo pre-clinical models in inflammation or oncology. A number of these inhibitors have progressed to the clinic where pharmacology-driven adverse events have been reported. To better understand the contribution of each domain to their efficacy and improve their safety profile, selective inhibitors are required. This article discloses the profile of GSK046, also known as iBET-BD2, a highly selective inhibitor of the second bromodomains of the BET proteins that has undergone extensive pre-clinical in vitro and in vivo characterization.

Published

2020

6. GSK789: A Selective Inhibitor of the First Bromodomains (BD1) of the Bromo and Extra Terminal Domain (BET) Proteins

Author

Peter Ernest Soden, Massimo Petretich, Robert J. Watson, Laurie J. Gordon, Chun-wa Chung, Paola Grandi, Alex Phillipou, Paul Bamborough, Emmanuel Hubert Demont, Rab K. Prinjha, Inmaculada Rioja, Thilo Werner, Robert E. Davis, and Heather A. Barnett

Subjects

Cellular activity, Anti-Inflammatory Agents, Cell Cycle Proteins, chemical and pharmacologic phenomena, Molecular Dynamics Simulation, Quinolones, Pharmacology, Crystallography, X-Ray, 01 natural sciences, 03 medical and health sciences, Protein Domains, In vivo, Cell Line, Tumor, Drug Discovery, Humans, Naphthyridines, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Binding Sites, Chemistry, hemic and immune systems, Highly selective, In vitro, 0104 chemical sciences, Bromodomain, DNA-Binding Proteins, 010404 medicinal & biomolecular chemistry, ATPases Associated with Diverse Cellular Activities, Molecular Medicine, Half-Life, Transcription Factors

Abstract

Pan-bromodomain and extra terminal (BET) inhibitors interact equipotently with all eight bromodomains of the BET family of proteins. They have shown profound efficacy in vitro and in vivo in oncology and immunomodulatory models, and a number of them are currently in clinical trials where significant safety signals have been reported. It is therefore important to understand the functional contribution of each bromodomain to assess the opportunity to tease apart efficacy and toxicity. This article discloses the in vitro and cellular activity profiles of GSK789, a potent, cell-permeable, and highly selective inhibitor of the first bromodomains of the BET family.

Published

2020

7. GSK973 Is an Inhibitor of the Second Bromodomains (BD2s) of the Bromodomain and Extra-Terminal (BET) Family

Author

Anne-Marie Michon, Rab K. Prinjha, Alex Preston, Laurie J. Gordon, Inmaculada Rioja, Pierre Thesmar, Emmanuel Hubert Demont, James Michael Woolven, Stephen John Atkinson, Jon T. Seal, Cassie Messenger, Lee Andrew Harrison, Paola Grandi, Darren Jason Mitchell, Robert J. Watson, Simon Taylor, Chun-wa Chung, James Gray, Antonia J. Lewis, Ian D. Wall, Dave Lugo, and Paul Bamborough

Subjects

010405 organic chemistry, business.industry, Organic Chemistry, chemical and pharmacologic phenomena, hemic and immune systems, Pharmacology, Highly selective, 01 natural sciences, Biochemistry, In vitro, 0104 chemical sciences, Bromodomain, 010404 medicinal & biomolecular chemistry, Safety profile, In vivo, Drug Discovery, Medicine, business

Abstract

[Image: see text] Pan-BET inhibitors have shown profound efficacy in a number of in vivo preclinical models and have entered the clinic in oncology trials where adverse events have been reported. These inhibitors interact equipotently with the eight bromodomains of the BET family of proteins. To better understand the contribution of each domain to their efficacy and to improve from their safety profile, selective inhibitors are required. This Letter discloses the profile of GSK973, a highly selective inhibitor of the second bromodomains of the BET proteins that has undergone extensive preclinical in vitro and in vivo characterization.

Published

2020

8. Optimization of a series of 2,3-dihydrobenzofurans as highly potent, second bromodomain (BD2)-selective, bromo and extra-terminal domain (BET) inhibitors

Author

Ian D. Wall, Thomas Grimes, Laurie J. Gordon, James Michael Woolven, Simon Taylor, Robert P. Davis, Simon C. C. Lucas, Chun-wa Chung, James J R Gray, Paola Grandi, Nicholas C. O. Tomkinson, Rab K. Prinjha, Robert J. Watson, Inmaculada Rioja, Alex Preston, Alexander N Phillipou, Stephen John Atkinson, and Emmanuel Hubert Demont

Subjects

RM, QL, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Proteins, Combinatorial chemistry, In vitro, Bromodomain, RS, Structure-Activity Relationship, Solubility, Pharmacokinetics, In vivo, Drug Discovery, Humans, Molecular Medicine, Selectivity, Benzofurans

Abstract

Herein, a series of 2,3-dihydrobenzofurans have been developed as highly potent bromo and extra-terminal domain (BET) inhibitors with 1000-fold selectivity for the second bromodomain (BD2) over the first bromodomain (BD1). Investment in the development of two orthogonal synthetic routes delivered inhibitors that were potent and selective but had raised in vitro clearance and suboptimal solubility. Insertion of a quaternary center into the 2,3-dihydrobenzofuran core blocked a key site of metabolism and improved the solubility. This led to the development of inhibitor 71 (GSK852): a potent, 1000-fold-selective, highly soluble compound with good in vivo rat and dog pharmacokinetics.

Published

2021

9. Fragment-based Scaffold Hopping: Identification of Potent, Selective, and Highly Soluble Bromo and Extra Terminal Domain (BET) Second Bromodomain (BD2) Inhibitors

Author

Alex Phillipou, Ryan G. Kruger, Simon Taylor, Chun-wa Chung, Rab K. Prinjha, Laurie J. Gordon, Robert J. Watson, James Gray, Alex Preston, James J. Foley, Cassie Messenger, Anna K. Bassil, Inmaculada Rioja, James Michael Woolven, Xi-Ping Zhang, Francesco Rianjongdee, Paola Grandi, Jeanne J. Matteo, Anastasia Wyce, Ian D. Wall, Paul Bamborough, Darren Jason Mitchell, Lee Andrew Harrison, Michael T. McCabe, Stephen John Atkinson, Jonathan Thomas Seal, and Emmanuel Hubert Demont

Subjects

Improved solubility, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Stereochemistry, Proteins, Pyrazole, Scaffold hopping, Bromodomain, chemistry.chemical_compound, Safety profile, Structure-Activity Relationship, Drug Discovery, Molecular Medicine, Humans, Pyrazoles, Furans, Pyrrole

Abstract

The profound efficacy of pan-BET inhibitors is well documented, but these epigenetic agents have shown pharmacology-driven toxicity in oncology clinical trials. The opportunity to identify inhibitors with an improved safety profile by selective targeting of a subset of the eight bromodomains of the BET family has triggered extensive medicinal chemistry efforts. In this article, we disclose the identification of potent and selective drug-like pan-BD2 inhibitors such as pyrazole 23 (GSK809) and furan 24 (GSK743) that were derived from the pyrrole fragment 6. We transpose the key learnings from a previous pyridone series (GSK620 2 as a representative example) to this novel class of inhibitors, which are characterized by significantly improved solubility relative to our previous research.

Published

2021

10. Optimization of Naphthyridones into Selective TATA-Binding Protein Associated Factor 1 (TAF1) Bromodomain Inhibitors

Author

Emmanuel Hubert Demont, Philip G. Humphreys, Alex Phillipou, Michael A. Clegg, Paul Bamborough, Peter D. Craggs, Chun-wa Chung, Rab K. Prinjha, Gemma Michele Liwicki, Nicholas C. O. Tomkinson, Natalie Hope Theodoulou, and Laurie J. Gordon

Subjects

biology, Chemistry, Organic Chemistry, Target engagement, Computational biology, Biochemistry, Small molecule, Bromodomain, TAF1, TA164, Drug Discovery, biology.protein, QD, Epigenetics, TATA-binding protein

Abstract

[Image: see text] Bromodomain containing proteins and the acetyl-lysine binding bromodomains contained therein are increasingly attractive targets for the development of novel epigenetic therapeutics. To help validate this target class and unravel the complex associated biology, there has been a concerted effort to develop selective small molecule bromodomain inhibitors. Herein we describe the structure-based efforts and multiple challenges encountered in optimizing a naphthyridone template into selective TAF1(2) bromodomain inhibitors which, while unsuitable as chemical probes themselves, show promise for the future development of small molecules to interrogate TAF1(2) biology. Key to this work was the introduction and modulation of the basicity of a pendant amine which had a substantial impact on not only bromodomain selectivity but also cellular target engagement.

Published

2021

11. Structure-based design of a bromodomain and extraterminal domain (BET) inhibitor selective for the N-terminal bromodomains that retains an anti-inflammatory and antiproliferative phenotype

Author

James M. Woolven, William J. Kerr, Chun-wa Chung, Bhumika Karamshi, Beata S. Wyspiańska, John Evans, Emmanuel Hubert Demont, Laurie Gordon, Matthew J Lindon, Peter E. Soden, Rob Willis, Leanne Cutler, Darren J. Mitchell, Christopher Roland Wellaway, Antonia J. Lewis, Robert J. Watson, Paul Bamborough, Simon Taylor, Inmaculada Rioja, Sharon G. Bernard, Rab K. Prinjha, and Peter D. Craggs

Subjects

Male, BRD4, medicine.drug_class, Anti-Inflammatory Agents, Cell Cycle Proteins, Molecular Dynamics Simulation, Quinolones, 01 natural sciences, Anti-inflammatory, BET inhibitor, 03 medical and health sciences, Mice, Protein Domains, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, QD, Epigenetics, Phylogeny, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Binding Sites, Small molecule, Phenotype, 0104 chemical sciences, Amino acid, Bromodomain, Cell biology, 010404 medicinal & biomolecular chemistry, chemistry, Drug Design, Leukocytes, Mononuclear, Molecular Medicine, Cytokines, Half-Life, Transcription Factors

Abstract

The bromodomain and extraterminal domain (BET) family of epigenetic regulators comprises four proteins (BRD2, BRD3, BRD4, BRDT), each containing tandem bromodomains. To date, small molecule inhibitors of these proteins typically bind all eight bromodomains of the family with similar affinity, resulting in a diverse range of biological effects. To enable further understanding of the broad phenotype characteristic of pan-BET inhibition, the development of inhibitors selective for individual, or sets of, bromodomains within the family is required. In this regard, we report the discovery of a potent probe molecule possessing up to 150-fold selectivity for the N-terminal bromodomains (BD1s) over the C-terminal bromodomains (BD2s) of the BETs. Guided by structural information, a specific amino acid difference between BD1 and BD2 domains was targeted for selective interaction with chemical functionality appended to the previously developed I-BET151 scaffold. Data presented herein demonstrate that selective inhibition of BD1 domains is sufficient to drive anti-inflammatory and antiproliferative effects.

Published

2020

12. The optimization of potent ATAD2 and CECR2 bromodomain inhibitors with an atypical binding mode

Author

Chun-wa Chung, Rab K. Prinjha, Simon C. C. Lucas, Nicholas C. O. Tomkinson, Alexander N Phillipou, Stephen John Atkinson, Darren Jason Mitchell, Paul Bamborough, Robert J. Sheppard, Emmanuel Hubert Demont, Robert J. Watson, Laurie J. Gordon, and Heather A. Barnett

Subjects

Stereochemistry, Lysine, 01 natural sciences, Protein Structure, Secondary, 03 medical and health sciences, Protein structure, Protein Domains, Drug Discovery, Humans, QD, Asparagine, Tyrosine, 030304 developmental biology, Sulfonamides, 0303 health sciences, biology, Chemistry, HEK 293 cells, 0104 chemical sciences, Bromodomain, DNA-Binding Proteins, 010404 medicinal & biomolecular chemistry, HEK293 Cells, Histone, Acetylation, biology.protein, ATPases Associated with Diverse Cellular Activities, Molecular Medicine, Protein Binding, Transcription Factors

Abstract

Most bromodomain inhibitors mimic the interactions of the natural acetylated lysine (KAc) histone substrate through key interactions with conserved asparagine and tyrosine residues within the binding pocket. Herein we report the optimization of a series of phenyl sulfonamides that exhibit a novel mode of binding to non-bromodomain and extra terminal domain (non-BET) bromodomains through displacement of a normally conserved network of four water molecules. Starting from an initial hit molecule, we report its divergent optimization toward the ATPase family AAA domain containing 2 (ATAD2) and cat eye syndrome chromosome region, candidate 2 (CECR2) domains. This work concludes with the identification of (R)-55 (GSK232), a highly selective, cellularly penetrant CECR2 inhibitor with excellent physicochemical properties.

Published

2020

13. Domain-selective targeting of BET proteins in cancer and immunological diseases

Author

Emmanuel Hubert Demont, Massimo Petretich, and Paola Grandi

Subjects

Cancer therapy, Inflammation, Antineoplastic Agents, Biochemistry, Analytical Chemistry, Small Molecule Libraries, Protein Domains, Neoplasms, Drug Discovery, medicine, Animals, Humans, Immunologic Factors, Epigenetics, Molecular Targeted Therapy, Effector, business.industry, Cell growth, Cancer, Proteins, medicine.disease, Bromodomain, Immune System Diseases, Cancer research, Immunological diseases, medicine.symptom, business

Abstract

Cancer and inflammation are strongly interconnected processes. Chronic inflammatory pathologies can be at the heart of tumor development; similarly, tumor-elicited inflammation is a consequence of many cancers. The mechanistic interdependence between cancer and inflammatory pathologies points toward common protein effectors which represent potential shared targets for pharmacological intervention. Epigenetic mechanisms often drive resistance to cancer therapy and immunomodulatory strategies. The bromodomain and extraterminal domain (BET) proteins are epigenetic adapters which play a major role in controlling cell proliferation and the production of inflammatory mediators. A plethora of small molecules aimed at inhibiting BET protein function to treat cancer and inflammatory diseases have populated academic and industry efforts in the last 10 years. In this review, we will discuss recent pharmacological approaches aimed at targeting a single or a subset of the eight bromodomains within the BET family which have the potential to tease apart clinical efficacy and safety signals of BET inhibitors.

Published

2019

14. A Qualified Success: Discovery of a New Series of ATAD2 Bromodomain Inhibitors with a Novel Binding Mode Using High-Throughput Screening and Hit Qualification

Author

Andrew D. Roberts, Peter Francis, Paola Grandi, Emma J. Jones, David P. Dixon, Robert J. Watson, Christina Rau, Peter Pogány, Angela Bridges, Chun-wa Chung, Darren Jason Mitchell, Rab K. Prinjha, Peter D. Craggs, Kelly Locke, Emmanuel Hubert Demont, Anne-Marie Michon, Bhumika Karamshi, Rebecca C. Furze, Paul Bamborough, Robert J. Sheppard, Simon C. C. Lucas, and Ana Maria Roa

Subjects

Models, Molecular, 0303 health sciences, Molecular Structure, Chemistry, High-throughput screening, Computational biology, 01 natural sciences, Biophysical Phenomena, 0104 chemical sciences, Bromodomain, High-Throughput Screening Assays, DNA-Binding Proteins, Small Molecule Libraries, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, Protein Domains, Catalytic Domain, Drug Design, Drug Discovery, Hit rate, Molecular Medicine, ATPases Associated with Diverse Cellular Activities, Humans, 030304 developmental biology, Protein Binding

Abstract

The bromodomain of ATAD2 has proved to be one of the least-tractable proteins within this target class. Here, we describe the discovery of a new class of inhibitors by high-throughput screening and show how the difficulties encountered in establishing a screening triage capable of finding progressible hits were overcome by data-driven optimization. Despite the prevalence of nonspecific hits and an exceptionally low progressible hit rate (0.001%), our optimized hit qualification strategy employing orthogonal biophysical methods enabled us to identify a single active series. The compounds have a novel ATAD2 binding mode with noncanonical features including the displacement of all conserved water molecules within the active site and a halogen-bonding interaction. In addition to reporting this new series and preliminary structure-activity relationship, we demonstrate the value of diversity screening to complement the knowledge-based approach used in our previous ATAD2 work. We also exemplify tactics that can increase the chance of success when seeking new chemical starting points for novel and less-tractable targets.

Published

2019

15. GSK6853, a Chemical Probe for Inhibition of the BRPF1 Bromodomain

Author

Laurie J. Gordon, David J. Fallon, Heather A. Barnett, Chun-wa Chung, Darren Jason Mitchell, Emma J. Jones, Robert J. Watson, Rab K. Prinjha, Armelle Le Gall, Isabelle Becher, Paola Grandi, Emmanuel Hubert Demont, Edward Hooper-Greenhill, Peter D. Craggs, Mark J. Bird, Allan J. B. Watson, Hawa Diallo, Robert P. Law, Robert J. Sheppard, Anne-Marie Michon, Dave Lugo, Paul Bamborough, and Clare I. Hobbs

Subjects

0301 basic medicine, Scaffold protein, biology, Protein family, 010405 organic chemistry, Organic Chemistry, Chemical probe, Histone acetyltransferase, 01 natural sciences, Biochemistry, Molecular biology, 0104 chemical sciences, Bromodomain, Cell biology, 03 medical and health sciences, 030104 developmental biology, Transcription (biology), In vivo, Drug Discovery, biology.protein, Epigenetics

Abstract

The BRPF (Bromodomain and PHD Finger-containing) protein family are important scaffolding proteins for assembly of MYST histone acetyltransferase complexes. A selective benzimidazolone BRPF1 inhibitor showing micromolar activity in a cellular target engagement assay was recently described. Herein, we report the optimization of this series leading to the identification of a superior BRPF1 inhibitor suitable for in vivo studies.

Published

2016

16. Aiming to Miss a Moving Target: Bromo and Extra Terminal Domain (BET) Selectivity in Constrained ATAD2 Inhibitors

Author

Rab K. Prinjha, Emmanuel Hubert Demont, Rebecca C. Furze, Chun-wa Chung, Robert J. Sheppard, Robert J. Watson, Heather A. Barnett, Christina Rau, Paul Bamborough, Anne-Marie Michon, Thilo Werner, Paola Grandi, and Darren Jason Mitchell

Subjects

0301 basic medicine, Models, Molecular, Protein Conformation, Druggability, Chemical probe, Cell Cycle Proteins, Small Molecule Libraries, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, 0302 clinical medicine, Protein Domains, Drug Discovery, Humans, Molecular Structure, Nuclear Proteins, Tropane, Combinatorial chemistry, Bromodomain, DNA-Binding Proteins, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Molecular Medicine, ATPases Associated with Diverse Cellular Activities, Piperidine, Selectivity, Transcription Factors

Abstract

ATAD2 is a cancer-associated protein whose bromodomain has been described as among the least druggable of its class. In our recent disclosure of the first chemical probe against this bromodomain, GSK8814 (6), we described the use of a conformationally constrained methoxy piperidine to gain selectivity over the BET bromodomains. Here we describe an orthogonal conformational restriction strategy of the piperidine ring to give potent and selective tropane inhibitors and show structural insights into why this was more challenging than expected. Greater understanding of why different rational approaches succeeded or failed should help in the future design of selectivity in the bromodomain family.

Published

2018

17. Discovery of Tetrahydroquinoxalines as Bromodomain and Extra-Terminal Domain (BET) Inhibitors with Selectivity for the Second Bromodomain

Author

David Jonathan Hirst, Chun-wa Chung, Rab K. Prinjha, Stephen John Atkinson, Robert P. Law, Paul Bamborough, Allan J. B. Watson, Emmanuel Hubert Demont, Matthew J Lindon, and Laurie J. Gordon

Subjects

0301 basic medicine, Models, Molecular, BRD4, Protein Conformation, Quantitative Structure-Activity Relationship, Sequence Homology, chemical and pharmacologic phenomena, Cell Cycle Proteins, Plasma protein binding, Molecular Dynamics Simulation, Protein Serine-Threonine Kinases, 01 natural sciences, 03 medical and health sciences, Protein structure, Quinoxalines, Drug Discovery, Humans, Protein Interaction Domains and Motifs, Amino Acid Sequence, Binding Sites, biology, Molecular Structure, 010405 organic chemistry, Drug discovery, Chemistry, Nuclear Proteins, hemic and immune systems, Combinatorial chemistry, 0104 chemical sciences, Bromodomain, 030104 developmental biology, Histone, Acetylation, biology.protein, Molecular Medicine, Selectivity, Protein Binding, Transcription Factors

Abstract

The bromodomain and extra-terminal domain (BET) family of proteins bind acetylated lysine residues on histone proteins. The four BET bromodomains—BRD2, BRD3, BRD4, and BRDT—each contain two bromodomain modules. BET bromodomain inhibition is a potential therapy for various cancers and immunoinflammatory diseases, but few reported inhibitors show selectivity within the BET family. Inhibitors with selectivity for the first or second bromodomain are desired to aid investigation of the biological function of these domains. Focused library screening identified a series of tetrahydroquinoxalines with selectivity for the second bromodomains of the BET family (BD2). Structure-guided optimization of the template improved potency, selectivity, and physicochemical properties, culminating in potent BET inhibitors with BD2 selectivity.

Published

2018

18. Navigating CYP1A Induction and Arylhydrocarbon Receptor Agonism in Drug Discovery. A Case History with S1P1 Agonists

Author

Aarti Patel, Nigel Deeks, Maxine A. Taylor, Jason Witherington, Dung Nguyen, Robert J. Watson, Rino A. Bit, Fiona McClure, Emmanuel Hubert Demont, James Gray, Holly Ashall, Steve R. Hood, and Simon Taylor

Subjects

Models, Molecular, Context (language use), Pharmacology, Rats, Sprague-Dawley, Mice, Structure-Activity Relationship, Dogs, Downregulation and upregulation, Cytochrome P-450 CYP1A2, In vivo, Drug Discovery, Cytochrome P-450 CYP1A1, Animals, Humans, RNA, Messenger, Receptor, biology, Drug discovery, Chemistry, Cytochrome P450, Lipids, In vitro, Rats, Up-Regulation, Macaca fascicularis, Receptors, Lysosphingolipid, Receptors, Aryl Hydrocarbon, Drug development, Drug Design, Enzyme Induction, Hepatocytes, biology.protein, Molecular Medicine

Abstract

This article describes the finding of substantial upregulation of mRNA and enzymes of the cytochrome P450 1A family during a lead optimization campaign for small molecule S1P1 agonists. Fold changes in mRNA up to 10,000-fold for CYP1A1 in vivo in rat and cynomolgus monkey and up to 45-fold for CYP1A1 and CYP1A2 in vitro in rat and human hepatocytes were observed. Challenges observed with correlating induction in vitro and induction in vivo resulted in the implementation of a short, 4 day in vivo screening study in the rat which successfully identified noninducers. Subtle structure-activity relationships in this series of S1P1 agonists are described extending beyond planarity and lipophilicity, and the impact and considerations of AhR and CYP1A induction in the context of drug development are discussed.

Published

2015

19. Structure-Based Optimization of Naphthyridones into Potent ATAD2 Bromodomain Inhibitors

Author

Emma J. Jones, David P. Dixon, Robert J. Watson, Chun-wa Chung, Anne-Marie Michon, Clement Douault, Emmanuel Hubert Demont, Paul Bamborough, Hawa Diallo, Thilo Werner, Christina Rau, Paola Grandi, Robert J. Sheppard, Rab K. Prinjha, Rebecca C. Furze, Bhumika Karamshi, Darren Jason Mitchell, and Heather A. Barnett

Subjects

Adenosine Triphosphatases, Models, Molecular, Molecular Structure, Chemistry, Stereochemistry, chemical and pharmacologic phenomena, hemic and immune systems, Bromodomain, DNA-Binding Proteins, Drug Discovery, ATPases Associated with Diverse Cellular Activities, Molecular Medicine, Structure based, Naphthyridines, Selectivity

Abstract

ATAD2 is a bromodomain-containing protein whose overexpression is linked to poor outcomes in a number of different cancer types. To date, no potent and selective inhibitors of the bromodomain have been reported. This article describes the structure-based optimization of a series of naphthyridones from micromolar leads with no selectivity over the BET bromodomains to inhibitors with sub-100 nM ATAD2 potency and 100-fold BET selectivity.

Published

2015

20. Optimization of Sphingosine-1-phosphate-1 Receptor Agonists: Effects of Acidic, Basic, and Zwitterionic Chemotypes on Pharmacokinetic and Pharmacodynamic Profiles

Author

Robert J. Watson, David Norton, John Skidmore, Christopher N. Johnson, Gerard Martin Paul Giblin, Jennifer Sweeting, Rivers Dean Andrew, Mahmood Ahmed, Andrea C. Haynes, Ian D. Wall, Sally Redshaw, Karen Louise Philpott, Jason Witherington, David N. Hurst, Umesh Kumar, James Myatt, Simon Taylor, Emmanuel Hubert Demont, Alexander J. Stevens, Tom D. Heightman, Rino A. Bit, D. Vesey, Jag Paul Heer, and Andrew Peter Cridland

Subjects

Male, Models, Molecular, Metabolite, Carboxylic Acids, Pharmacology, Structure-Activity Relationship, chemistry.chemical_compound, Pharmacokinetics, Heterocyclic Compounds, In vivo, Drug Discovery, medicine, Animals, Structure–activity relationship, Lymphocytes, Sphingosine-1-phosphate, Receptor, Cells, Cultured, Molecular Structure, Chemistry, Fingolimod, In vitro, Receptors, Lysosphingolipid, Biochemistry, Rats, Inbred Lew, Molecular Medicine, Immunosuppressive Agents, medicine.drug

Abstract

The efficacy of the recently approved drug fingolimod (FTY720) in multiple sclerosis patients results from the action of its phosphate metabolite on sphingosine-1-phosphate S1P1 receptors, while a variety of side effects have been ascribed to its S1P3 receptor activity. Although S1P and phospho-fingolimod share the same structural elements of a zwitterionic headgroup and lipophilic tail, a variety of chemotypes have been found to show S1P1 receptor agonism. Here we describe a study of the tolerance of the S1P1 and S1P3 receptors toward bicyclic heterocycles of systematically varied shape and connectivity incorporating acidic, basic, or zwitterionic headgroups. We compare their physicochemical properties, their performance in in vitro and in vivo pharmacokinetic models, and their efficacy in peripheral lymphocyte lowering. The campaign resulted in the identification of several potent S1P1 receptor agonists with good selectivity vs S1P3 receptors, efficacy at

Published

2014

21. The Discovery of I-BET726 (GSK1324726A), a Potent Tetrahydroquinoline ApoA1 Up-Regulator and Selective BET Bromodomain Inhibitor

Author

Chun-wa Chung, Rab K. Prinjha, Rejbinder Kaur, Peter Ernest Soden, Ann Louise Walker, Van Loc Nguyen, Christophe Simon, Simon Taylor, Romain Luc Marie Gosmini, Jean-Marie Brusq, Antonia J. Lewis, Mark B. Schilling, Lionel Trottet, Matthew D. Walker, Leanne Cutler, Olivier Mirguet, Emmanuel Hubert Demont, Edwige Nicodeme, Eric Boursier, Jérôme Toum, Alizon M. Riou-Eymard, Gael Krysa, Hugh Clark, and Paul Bamborough

Subjects

Anti-Inflammatory Agents, Regulator, Cell Cycle Proteins, Inflammation, Protein Serine-Threonine Kinases, Benzoates, Mice, Structure-Activity Relationship, Transcription (biology), Neuroblastoma, Drug Discovery, medicine, Animals, Humans, Histone code, Epigenetics, Gene, Genetics, Apolipoprotein A-I, Chemistry, Nuclear Proteins, medicine.disease, Bromodomain, Aminoquinolines, Quinolines, Cancer research, Molecular Medicine, medicine.symptom, Transcription Factors

Abstract

Through their function as epigenetic readers of the histone code, the BET family of bromodomain-containing proteins regulate expression of multiple genes of therapeutic relevance, including those involved in tumor cell growth and inflammation. BET bromodomain inhibitors have profound antiproliferative and anti-inflammatory effects which translate into efficacy in oncology and inflammation models, and the first compounds have now progressed into clinical trials. The exciting biology of the BETs has led to great interest in the discovery of novel inhibitor classes. Here we describe the identification of a novel tetrahydroquinoline series through up-regulation of apolipoprotein A1 and the optimization into potent compounds active in murine models of septic shock and neuroblastoma. At the molecular level, these effects are produced by inhibition of BET bromodomains. X-ray crystallography reveals the interactions explaining the structure-activity relationships of binding. The resulting lead molecule, I-BET726, represents a new, potent, and selective class of tetrahydroquinoline-based BET inhibitors.

Published

2014

22. 1,3-Dimethyl Benzimidazolones Are Potent, Selective Inhibitors of the BRPF1 Bromodomain

Author

Emmanuel Hubert Demont, Robert J. Sheppard, Paola Grandi, Clare I. Hobbs, Chun-wa Chung, Peter D. Craggs, Jameed Hussain, Darren Jason Mitchell, Laurie J. Gordon, Paul Bamborough, Armelle Le Gall, David J. Fallon, Andrew D. Roberts, Rab K. Prinjha, Emma J. Jones, Robert J. Watson, and Anne-Marie Michon

Subjects

Scaffold protein, Protein family, biology, Chemistry, Organic Chemistry, Chemical probe, Histone acetyltransferase, Biochemistry, Bromodomain, body regions, Transcription (biology), Drug Discovery, Cancer research, biology.protein, Epigenetics

Abstract

The BRPF (bromodomain and PHD finger-containing) protein family are important scaffolding proteins for assembly of MYST histone acetyltransferase complexes. Here, we report the discovery, binding mode, and structure-activity relationship (SAR) of the first potent, selective series of inhibitors of the BRPF1 bromodomain.

Published

2014

23. Discovery of Tetrahydropyrazolopyridine as Sphingosine 1-Phosphate Receptor 3 (S1P3)-Sparing S1P1 Agonists Active at Low Oral Doses

Author

Nigel Deeks, Robert J. Watson, James Matthew Bailey, Simon Taylor, Jessica F. Renaux, Andrea C. Haynes, Simon J. Dowell, Rino A. Bit, Colin David Eldred, Colin A. Campbell, Duncan S. Holmes, Jason Witherington, Umesh Kumar, Jack A. Brown, Mary A. Morse, Emmanuel Hubert Demont, Pam Gaskin, Chris A. Smethurst, Gail A. Seal, Greg J. Osborne, James Gray, Robert Willis, and David Jonathan Hirst

Subjects

0301 basic medicine, Agonist, Drug, Male, medicine.drug_class, Pyridines, media_common.quotation_subject, Administration, Oral, Mice, Inbred Strains, Pharmacology, 01 natural sciences, Cell Line, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Dogs, Drug Discovery, medicine, Structure–activity relationship, Animals, Humans, Receptor, Sphingosine-1-Phosphate Receptors, media_common, Sphingosine 1-Phosphate Receptor 3, Dose-Response Relationship, Drug, Molecular Structure, Drug discovery, Chemistry, Tetrahydroisoquinoline, 0104 chemical sciences, Rats, 010404 medicinal & biomolecular chemistry, Receptors, Lysosphingolipid, 030104 developmental biology, Rats, Inbred Lew, THIQ, Molecular Medicine, Pyrazoles, medicine.drug

Abstract

FTY720 is the first oral small molecule approved for the treatment of people suffering from relapsing-remitting multiple sclerosis. It is a potent agonist of the S1P1 receptor, but its lack of selectivity against the S1P3 receptor has been linked to most of the cardiovascular side effects observed in the clinic. These findings have triggered intensive efforts toward the identification of a second generation of S1P3-sparing S1P1 agonists. We have recently disclosed a series of orally active tetrahydroisoquinoline (THIQ) compounds matching these criteria. In this paper we describe how we defined and implemented a strategy aiming at the discovery of selective structurally distinct follow-up agonists. This effort culminated with the identification of a series of orally active tetrahydropyrazolopyridines.

Published

2016

24. The utility of pharmacokinetic–pharmacodynamic modeling in the discovery and optimization of selective S1P1agonists

Author

Nigel Deeks, Karen Leavens, Aarti Patel, Colin A. Campbell, Helen Garden, Jenni Cryan, Emmanuel Hubert Demont, Simon Taylor, Jason Witherington, Pam Gaskin, Andrea C. Haynes, Simon J. Dowell, Robert Willis, James Gray, and Mary A. Morse

Subjects

Male, Agonist, medicine.drug_class, Health, Toxicology and Mutagenesis, Pharmacology, Biology, Toxicology, Biochemistry, Multiple Sclerosis, Relapsing-Remitting, Pharmacokinetics, GTP-Binding Proteins, Sphingosine, In vivo, medicine, Animals, Potency, Lymphocytes, PK/PD models, Arrestin, Fingolimod Hydrochloride, Drug discovery, Rats, Inbred Strains, General Medicine, Fingolimod, Rats, Propylene Glycols, Pharmacodynamics, Lysophospholipids, Signal Transduction, medicine.drug

Abstract

Sphingosine-1-phosphate (S1P(1)) receptor agonists such as Fingolimod (FTY-720) are a novel class of immunomodulators that have clinical utility in the treatment of remitting relapsing multiples sclerosis. This class of compound act by inducing peripheral lymphopenia. Using an integrated pharmacokinetic/pharmacodynamic (PK-PD) approach based on an in vivo rat model, novel S1P(1) agonists were identified with a predicted more rapid rate of reversibility of lymphocyte reduction in human compared to Fingolimod. The in vivo potency of 15 compounds based on PK-PD modelling of the rat lymphocyte reduction model was correlated with in vitro measures of potency at the S1P(1) receptor using β arrestin recruitment and G-protein signalling. A structurally novel S1P(1) agonist was identified and predictions of human pharmacokinetics and clinical dose are presented.

Published

2012

25. Discovery of a Brain-Penetrant S1P3-Sparing Direct Agonist of the S1P1 and S1P5 Receptors Efficacious at Low Oral Dose

Author

Karen Louise Philpott, Robert J. Watson, Jason Witherington, Greg J. Osborne, Terry Panchal, Simon Taylor, Nigel Deeks, Tom D. Heightman, James Gray, Umesh Kumar, Simon J. Dowell, Pam Gaskin, Lee Andrew Harrison, Robert Willis, Colin A. Campbell, Sandra Arpino, Sapna Desai, Rino A. Bit, Mary A. Morse, Emmanuel Hubert Demont, Andrea C. Haynes, Philip G. Humphreys, and Duncan S. Holmes

Subjects

Agonist, medicine.drug_class, Chemistry, organic chemicals, Multiple sclerosis, Central nervous system, Pharmacology, medicine.disease, Fingolimod, Therapeutic index, medicine.anatomical_structure, In vivo, Drug Discovery, medicine, Molecular Medicine, Potency, lipids (amino acids, peptides, and proteins), Receptor, medicine.drug

Abstract

2-Amino-2-(4-octylphenethyl)propane-1,3-diol 1 (fingolimod, FTY720) has been recently marketed in the United States for the treatment of patients with remitting relapsing multiple sclerosis (RRMS). Its efficacy has been primarily linked to the agonism on T cells of S1P(1), one of the five sphingosine 1-phosphate (S1P) G-protein-coupled receptors, while its cardiovascular side effects have been associated with activity at S1P(3). Emerging data suggest that the ability of this molecule to cross the blood-brain barrier and to interact with both S1P(1) and S1P(5) in the central nervous system (CNS) may contribute to its efficacy in treating patients with RRMS. We have recently disclosed the structure of an advanced, first generation S1P(3)-sparing S1P(1) agonist, a zwitterion with limited CNS exposure. In this Article, we highlight our strategy toward the identification of CNS-penetrant S1P(3)-sparing S1P(1) and S1P(5) agonists resulting in the discovery of 5-(3-{2-[2-hydroxy-1-(hydroxymethyl)ethyl]-5-methyl-1,2,3,4-tetrahydro-6-isoquinolinyl}-1,2,4-oxadiazol-5-yl)-2-[(1-methylethyl)oxy]benzonitrile 15. Its exceptional in vivo potency and good pharmacokinetic properties translate into a very low predicted therapeutic dose in human (

Published

2011

26. Discovery of a Selective S1P1 Receptor Agonist Efficacious at Low Oral Dose and Devoid of Effects on Heart Rate

Author

Andrea C. Haynes, Benjamin I. Andrews, Bela Rajiv Patel, Jason Witherington, Mary A. Morse, Umesh Kumar, Colin A. Campbell, Pam Gaskin, Sapna Desai, Robert Willis, Jason W. B. Cooke, Greg J. Osborne, Simon Taylor, Robert J. Watson, Terry Panchal, Alcide Perboni, Nigel Deeks, James Gray, Simon J. Dowell, Duncan S. Holmes, Rino A. Bit, and Emmanuel Hubert Demont

Subjects

Agonist, Bradycardia, medicine.medical_specialty, Sphingosine, medicine.drug_class, business.industry, Multiple sclerosis, Organic Chemistry, Arthritis, Pharmacology, medicine.disease, Biochemistry, Fingolimod, chemistry.chemical_compound, Endocrinology, chemistry, Pharmacokinetics, Internal medicine, Drug Discovery, medicine, medicine.symptom, business, Receptor, medicine.drug

Abstract

Gilenya (fingolimod, FTY720) was recently approved by the U.S. FDA for the treatment of patients with remitting relapsing multiple sclerosis (RRMS). It is a potent agonist of four of the five sphingosine 1-phosphate (S1P) G-protein-coupled receptors (S1P1 and S1P3-5). It has been postulated that fingolimod's efficacy is due to S1P1 agonism, while its cardiovascular side effects (transient bradycardia and hypertension) are due to S1P3 agonism. We have discovered a series of selective S1P1 agonists, which includes 3-[6-(5-{3-cyano-4-[(1-methylethyl)oxy]phenyl}-1,2,4-oxadiazol-3-yl)-5-methyl-3,4-dihydro-2(1H)-isoquinolinyl]propanoate, 20, a potent, S1P3-sparing, orally active S1P1 agonist. Compound 20 is as efficacious as fingolimod in a collagen-induced arthritis model and shows excellent pharmacokinetic properties preclinically. Importantly, the selectivity of 20 against S1P3 is responsible for an absence of cardiovascular signal in telemetered rats, even at high dose levels.

Published

2011

27. BACE-1 hydroxyethylamine inhibitors using novel edge-to-face interaction with Arg-296

Author

Alan Naylor, Emmanuel Hubert Demont, P. Theobald, Daryl S. Walter, G. Maile, Gareth Wayne, Ishrut Hussain, Colin Dingwall, B. Clarke, C. Howes, Sharon Sweitzer, D. Vesey, Leanne Cutler, Julie Hawkins, Rosalie Matico, J. Mosley, A. O'Brien, Virginie Soleil, Sally Redshaw, Kathrine J. Smith, Paul Rowland, and R. Dunsdon

Subjects

Molecular model, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Pharmaceutical Science, Carboxamide, Arginine, Crystallography, X-Ray, Biochemistry, Structure-Activity Relationship, Alzheimer Disease, Drug Discovery, Ethylamines, Amyloid precursor protein, medicine, Animals, Structure–activity relationship, Computer Simulation, Protease Inhibitors, Binding site, Molecular Biology, chemistry.chemical_classification, Binding Sites, biology, Organic Chemistry, Rats, Enzyme, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases, Amyloid precursor protein secretase

Abstract

Inhibition of the aspartyl protease BACE-1 has the potential to deliver a disease-modifying therapy for Alzheimer's disease. Herein, is described a series of potent inhibitors based on an hydroxyethylamine (HEA) transition state mimetic template. These inhibitors interact with the non prime side of the enzyme using a novel edge-to-face interaction with Arg-296.

Published

2010

28. Synthesis and structure–activity relationships of a series of (1H-pyrazol-4-yl)acetamide antagonists of the P2X7 receptor

Author

Shilina Roman, Anton D. Michel, P. Theobald, Daryl S. Walter, Livermore David, Alexander J. Stevens, Elena Fonfria, Andrew P. Moses, Emmanuel Hubert Demont, David John Davies, Robert Gleave, Mythily Vimal, Laura J. Chambers, Stefan Senger, and Paul John Beswick

Subjects

Stereochemistry, medicine.drug_class, Clinical Biochemistry, Administration, Oral, Pharmaceutical Science, Carboxamide, Biochemistry, Chemical synthesis, Compound 32, Structure-Activity Relationship, chemistry.chemical_compound, Anti-Infective Agents, Acetamides, Drug Discovery, Purinergic P2 Receptor Antagonists, medicine, Animals, Humans, Potency, Molecular Biology, Receptors, Purinergic P2, Chemistry, Organic Chemistry, Antagonist, Receptor antagonist, In vitro, High-Throughput Screening Assays, Rats, Injections, Intravenous, Pyrazoles, Molecular Medicine, Receptors, Purinergic P2X7, Acetamide

Abstract

High-throughput screening identified compound 1 as a potent P2X(7) receptor antagonist suitable for lead optimisation. Structure-activity relationships (SAR) of a series of (1H-pyrazol-4-yl)acetamides were investigated and compound 32 was identified as a potent P2X(7) antagonist with enhanced potency and favourable physicochemical and pharmacokinetic properties.

Published

2010

29. Second generation of BACE-1 inhibitors part 2: Optimisation of the non-prime side substituent

Author

D. Vesey, B. Clarke, Sharon Sweitzer, Julie Hawkins, A. O'Brien, Alan Naylor, J. Mosley, Nicolas Charrier, Julia A. Hubbard, G. Maile, Ishrut Hussain, Virginie Soleil, Paul Rowland, Kathrine J. Smith, Rosalie Matico, Colin Dingwall, Daryl S. Walter, R. Dunsdon, Gareth Wayne, P. Theobald, Emmanuel Hubert Demont, and Sally Redshaw

Subjects

Molecular model, Stereochemistry, Clinical Biochemistry, Thiazines, Substituent, Administration, Oral, Pharmaceutical Science, Pharmacology, Crystallography, X-Ray, Biochemistry, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Animal model, Alzheimer Disease, Drug Discovery, Ethylamines, medicine, Amyloid precursor protein, Animals, Aspartic Acid Endopeptidases, Humans, Structure–activity relationship, Computer Simulation, Protease Inhibitors, Molecular Biology, Amyloid beta-Peptides, Binding Sites, biology, Organic Chemistry, medicine.disease, First generation, Rats, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Alzheimer's disease

Abstract

Our first generation of hydroxyethylamine transition-state mimetic BACE-1 inhibitors allowed us to validate BACE-1 as a key target for Alzheimer's disease by demonstrating amyloid lowering in an animal model, albeit at rather high doses. Finding a molecule from this series which was active at lower oral doses proved elusive and demonstrated the need to find a novel series of inhibitors with improved pharmacokinetics. This Letter describes the discovery of such inhibitors.

Published

2009

30. Investigation of the scope of an enantioselective Co-mediated O→C rearrangement reaction

Author

Joseph P. A. Harrity, Simon J. Meek, and Emmanuel Hubert Demont

Subjects

Scope (project management), Chemistry, Stereochemistry, Organic Chemistry, Drug Discovery, Enantioselective synthesis, Moiety, Rearrangement reaction, General Medicine, Lewis acids and bases, Biochemistry

Abstract

A series of enantiomerically enriched functionalised pyrans bearing a dicobalt hexacarbonyl-alkyne moiety have been subjected to a Lewis acid mediated rearrangement to carbocyclic ketones. This process was found to provide cyclohexanones with good enantioselectivity, however, cyclobutanones were generated with complete loss of enantiocontrol.

Published

2007

31. Fragment-Based Discovery of Low-Micromolar ATAD2 Bromodomain Inhibitors

Author

Andrew D. Roberts, Bhumika Karamshi, Angela Bridges, Hawa Diallo, Chun-wa Chung, Kelly Locke, Peter D. Craggs, Darren Jason Mitchell, Paul Bamborough, Amanda Emmons, Christopher Roland Wellaway, Emma J. Jones, David P. Dixon, Robert J. Watson, Nathalie Barrett, Emmanuel Hubert Demont, Clement Douault, Robert J. Sheppard, Rab K. Prinjha, Rebecca C. Furze, Anne-Marie Michon, Paola Grandi, and Bernadette Mouzon

Subjects

Adenosine Triphosphatases, Models, Molecular, biology, Chemistry, Drug discovery, ATPase, Molecular Sequence Data, Cancer, Antineoplastic Agents, Quinolones, medicine.disease, Bromodomain, Protein Structure, Tertiary, Protein structure, Biochemistry, Disease severity, Drug Discovery, medicine, biology.protein, Cancer research, Molecular Medicine, Humans, Amino Acid Sequence, Enzyme Inhibitors, Peptide sequence

Abstract

Overexpression of ATAD2 (ATPase family, AAA domain containing 2) has been linked to disease severity and progression in a wide range of cancers, and is implicated in the regulation of several drivers of cancer growth. Little is known of the dependence of these effects upon the ATAD2 bromodomain, which has been categorized as among the least tractable of its class. The absence of any potent, selective inhibitors limits clear understanding of the therapeutic potential of the bromodomain. Here, we describe the discovery of a hit from a fragment-based targeted array. Optimization of this produced the first known micromolar inhibitors of the ATAD2 bromodomain.

Published

2015

32. From serine to functionalized enantiopure tetrahydroisoquinolines

Author

Stephen Hanessian, Emmanuel Hubert Demont, and Willem A. L. van Otterlo

Subjects

Serine, chemistry.chemical_compound, Enantiopure drug, chemistry, Intramolecular force, Organic Chemistry, Drug Discovery, Condensation, Biochemistry, Friedel–Crafts reaction, Isocyanate, Medicinal chemistry

Abstract

The reaction of γ-amino-α,β-unsaturated esters prepared from l -serine with diversely substituted arylcuprates affords the corresponding syn -adducts. Transformation of the amino group to an isocyanate, followed by Friedel–Crafts intramolecular condensation, leads to enantiopure 3,4-disubstituted tetrahydroisoquinolin-1-ones, which can be reduced to the corresponding tetrahydroisoquinolines.

Published

2000

33. Discovery of biaryl inhibitors of H+/K+ ATPase

Author

Gail Hutley, Nicholas Bailey, Neil Stuart Garton, Mark James Bamford, Gianpaolo Bravi, Irene Farre-Gutierrez, Pickering Paula Louise, and Emmanuel Hubert Demont

Subjects

Imidazopyridine, Hydrogen bond, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Imidazoles, Pharmaceutical Science, Proton Pump Inhibitors, H(+)-K(+)-Exchanging ATPase, Ring (chemistry), Biochemistry, chemistry.chemical_compound, Structure-Activity Relationship, chemistry, Intramolecular force, Drug Discovery, Molecular Medicine, Structure–activity relationship, Imidazole, Pharmacophore, Molecular Biology

Abstract

We report the identification of a novel biaryl template for H(+)/K(+) ATPase inhibition. Evaluation of critical SAR features within the biaryl imidazole framework and the use of pharmacophore modelling against known imidazopyridine and azaindole templates suggested that the geometry of the molecule is key to achieving activity. Herein we present our work optimising the potency of the molecule through modifications and substitutions to each of the ring systems. In particular sub-micromolar potency is achieved with (4b) presumably through a proposed intramolecular hydrogen bond that ensures the required imidazole basic centre is appropriately located.

Published

2009

34. Orally active C-6 heteroaryl- and heterocyclyl-substituted imidazo[1,2-a]pyridine acid pump antagonists (APAs)

Author

Andrew K. Takle, Gail Hutley, Neil Stuart Garton, Terry Panchal, Thomas George Christopher Hayhow, Emmanuel Hubert Demont, Delphine Brissy, Mark James Bamford, Irene Farre-Gutierrez, Joanna Brookfield, Nicholas Bailey, Richard L. Elliott, David J. Spalding, Antoinette Naylor, and Hui-Xian Seow

Subjects

Stereochemistry, Pyridines, Clinical Biochemistry, Pharmaceutical Science, Administration, Oral, Biochemistry, Chemical synthesis, chemistry.chemical_compound, H(+)-K(+)-Exchanging ATPase, Structure-Activity Relationship, Dogs, Pharmacokinetics, In vivo, Oral administration, Drug Discovery, Pyridine, Animals, Humans, Molecular Biology, biology, Organic Chemistry, Proton Pump Inhibitors, Hydrogen-Ion Concentration, Rats, Orally active, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Gastric acid

Abstract

Acid pump antagonists (APAs) such as the imidazo[1,2-a]pyridine AZD-0865 2 have proven efficacious at low oral doses in acid related gastric disorders. Herein we describe some of the broader SAR in this class of molecule and detail the discovery of an imidazo[1,2-a]pyridine 15 which has excellent efficacy in animal models of gastric acid secretion following oral administration, as well as a good overall developability profile. The discovery strategy focuses on use of heteroaryl and heterocyclic substituents at the C-6 position and optimization of developability characteristics through modulation of global physico-chemical properties.

Published

2009

35. Second generation of BACE-1 inhibitors part 3: Towards non hydroxyethylamine transition state mimetics

Author

Ishrut Hussain, G. Maile, A. O'Brien, Gareth Wayne, Julie Hawkins, Daryl S. Walter, Sharon Sweitzer, Virginie Soleil, B. Clarke, P. Theobald, Colin Dingwall, Emmanuel Hubert Demont, Alan Naylor, Paul Rowland, Rosalie Matico, Kathrine J. Smith, Leanne Cutler, J. Mosley, C. Howes, Sally Redshaw, R. Dunsdon, Julia A. Hubbard, Nicolas Charrier, and D. Vesey

Subjects

Molecular model, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Biological Availability, Biochemistry, Mice, Structure-Activity Relationship, Animal model, Dogs, Drug Discovery, Amyloid precursor protein, Ethylamines, Structure–activity relationship, Animals, Aspartic Acid Endopeptidases, Protease Inhibitors, ATP Binding Cassette Transporter, Subfamily B, Member 1, Molecular Biology, Mice, Knockout, Amyloid beta-Peptides, biology, Chemistry, Organic Chemistry, Biological activity, Combinatorial chemistry, First generation, Bioavailability, Rats, Enzyme inhibitor, biology.protein, Molecular Medicine

Abstract

Our first generation of hydroxyethylamine BACE-1 inhibitors proved unlikely to provide molecules that would lower amyloid in an animal model at low oral doses. This observation led us to the discovery of a second generation of inhibitors having nanomolar activity in a cell-based assay and with the potential for improved pharmacokinetic profiles. In this Letter, we describe our successful strategy for the optimization of oral bioavailability and also give insights into the design of compounds with the potential for improved brain penetration.

Published

2009

36. Second generation of BACE-1 inhibitors. Part 1: The need for improved pharmacokinetics

Author

B. Clarke, Paul Rowland, Sharon Sweitzer, D. Vesey, G. Maile, Rosalie Matico, Virginie Soleil, A. O'Brien, Sally Redshaw, Daryl S. Walter, Nicolas Charrier, Alan Naylor, J. Mosley, Julie Hawkins, Gareth Wayne, Emmanuel Hubert Demont, R. Dunsdon, Leanne Cutler, Kathrine J. Smith, P. Theobald, Julia A. Hubbard, Colin Dingwall, C. Howes, and Ishrut Hussain

Subjects

Amyloid, Clinical Biochemistry, Thiazines, Pharmaceutical Science, Administration, Oral, Pharmacology, Biochemistry, Mice, Structure-Activity Relationship, Pharmacokinetics, In vivo, Alzheimer Disease, Drug Discovery, medicine, Amyloid precursor protein, Ethylamines, Structure–activity relationship, Animals, Aspartic Acid Endopeptidases, Humans, Computer Simulation, Protease Inhibitors, Molecular Biology, Amyloid beta-Peptides, Binding Sites, biology, Chemistry, Organic Chemistry, medicine.disease, In vitro, Rats, Enzyme inhibitor, biology.protein, Molecular Medicine, Alzheimer's disease

Abstract

Inhibition of the aspartyl protease BACE-1 has the potential to deliver a disease-modifying therapy for Alzheimer's disease. We have recently disclosed a series of transition-state mimetic BACE-1 inhibitors showing nanomolar potency in cell-based assays. Amongst them, GSK188909 (compound 2) had favorable pharmacokinetics and was the first orally bioavailable inhibitor reported to demonstrate brain amyloid lowering in an animal model. In this Letter, we describe the reasons that led us to favor a second generation of inhibitors for further in vivo studies.

Published

2009

37. Second generation of hydroxyethylamine BACE-1 inhibitors: optimizing potency and oral bioavailability

Author

D. Vesey, Alan Naylor, Rosalie Matico, P. Jeffrey, Daryl S. Walter, Nicolas Charrier, Julie Hawkins, Sharon Sweitzer, B. Clarke, Paul Rowland, Ishrut Hussain, R. Dunsdon, A. O'Brien, Philip East, Colin Dingwall, Virginie Soleil, J. Mosley, Emmanuel Hubert Demont, Leanne Cutler, Sally Redshaw, Kathrine J. Smith, C. Howes, P. Theobald, G. Maile, and Gareth Wayne

Subjects

Models, Molecular, medicine.drug_class, Administration, Oral, Biological Availability, Carboxamide, Pharmacology, Benzothiadiazines, Structure-Activity Relationship, Dogs, In vivo, Oral administration, Drug Discovery, medicine, Ethylamines, Potency, Animals, Cell potency, chemistry.chemical_classification, biology, Bioavailability, Cyclic S-Oxides, Rats, chemistry, Biochemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Amyloid Precursor Protein Secretases, Tricyclic

Abstract

BACE-1 inhibition has the potential to provide a disease-modifying therapy for the treatment of Alzheimer’s disease. Optimization of a first generation of BACE-1 inhibitors led to the discovery of novel hydroxyethylamines (HEAs) bearing a tricyclic nonprime side. These derivatives have nanomolar cell potency and are orally bioavailable.

Published

2008

38. BACE-1 inhibitors part 2: identification of hydroxy ethylamines (HEAs) with reduced peptidic character

Author

Alan Naylor, R. Dunsdon, A. O'Brien, Rosalie Matico, Paul Rowland, Daryl S. Walter, Sharon Sweitzer, P. Theobald, Peter Henry Milner, Sally Redshaw, Gareth Wayne, G. Maile, B. Clarke, D. Vesey, David MacPherson, Emmanuel Hubert Demont, Kathrine J. Smith, J. Mosley, Andrew Faller, Ishrut Hussain, Ward John Gerard, Virginie Soleil, Julie Hawkins, Steven J. Stanway, Geoffrey Stemp, Colin Dingwall, and David R. Riddell

Subjects

Stereochemistry, medicine.drug_class, Clinical Biochemistry, Ethylamines, Pharmaceutical Science, Carboxamide, Stereoisomerism, Crystallography, X-Ray, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Amyloid beta-Protein Precursor, Structure-Activity Relationship, Alzheimer Disease, Drug Discovery, Hydrolase, medicine, Structure–activity relationship, Aspartic Acid Endopeptidases, Combinatorial Chemistry Techniques, Humans, Molecular Biology, biology, Molecular Structure, Chemistry, Organic Chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Ethylamine, Amyloid Precursor Protein Secretases

Abstract

This paper describes the discovery of non-peptidic, potent, and selective hydroxy ethylamine (HEA) inhibitors of BACE-1 by replacement of the prime side of a lead di-amide 2 . Inhibitors with nanosmolar potency and high selectivity were identified. Depending on the nature of the P 1 ′ and P 2 ′ substituents, two different binding modes were observed in X-ray co-crystal structures.

Published

2007

39. BACE-1 inhibitors part 3: identification of hydroxy ethylamines (HEAs) with nanomolar potency in cells

Author

Steven J. Stanway, Alistair Stuart, John Skidmore, Sally Redshaw, Rosalie Matico, Geoffrey Stemp, Paul Rowland, A. O'Brien, Daryl S. Walter, Nicolas Charrier, Christopher N. Johnson, David R. Riddell, Peter Henry Milner, Sharon Sweitzer, Kathrine J. Smith, Gareth Wayne, Alan Naylor, Paul John Beswick, Colin Dingwall, Ward John Gerard, Julie Hawkins, J. Mosley, David MacPherson, P. Theobald, Emmanuel Hubert Demont, D. Vesey, Andrew Faller, G. Maile, Virginie Soleil, Robert Gleave, R. Dunsdon, Ishrut Hussain, and B. Clarke

Subjects

Stereochemistry, medicine.drug_class, Clinical Biochemistry, Ethylamines, Substituent, Pharmaceutical Science, Carboxamide, Crystallography, X-Ray, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Amyloid beta-Protein Precursor, Mice, Structure-Activity Relationship, Alzheimer Disease, Drug Discovery, medicine, Structure–activity relationship, Potency, Animals, Aspartic Acid Endopeptidases, Combinatorial Chemistry Techniques, Nanotechnology, Molecular Biology, biology, Molecular Structure, Organic Chemistry, Fluorine, Disease Models, Animal, chemistry, Enzyme inhibitor, biology.protein, Molecular Medicine, Ethylamine, Asparagine

Abstract

This article is focusing on further optimization of previously described hydroxy ethylamine (HEA) BACE-1 inhibitors obtained from a focused library with the support of X-ray crystallography. Optimization of the non-prime side of our inhibitors and introduction of a 6-membered sultam substituent binding to Asn-294 as well as a fluorine in the C-2 position led to derivatives with nanomolar potency in cell-based assays.

Published

2007

40. BACE-1 inhibitors part 1: identification of novel hydroxy ethylamines (HEAs)

Author

Paul Rowland, J. Mosley, Sally Redshaw, Ishrut Hussain, Peter Henry Milner, Rosalie Matico, Gareth Wayne, Colin Dingwall, Andrew Faller, Geoffrey Stemp, Emmanuel Hubert Demont, Kathrine J. Smith, P. Theobald, David MacPherson, B. Clarke, G. Maile, R. Dunsdon, David R. Riddell, Alan Naylor, Daryl S. Walter, Julie Hawkins, D. Vesey, Virginie Soleil, A. O'Brien, Sharon Sweitzer, Steven J. Stanway, and Ward John Gerard

Subjects

Amyloid, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Ethylamines, Pharmaceutical Science, Carboxamide, Crystallography, X-Ray, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Amyloid beta-Protein Precursor, Structure-Activity Relationship, Alzheimer Disease, Drug Discovery, Amyloid precursor protein, medicine, Aspartic Acid Endopeptidases, Combinatorial Chemistry Techniques, Molecular Biology, chemistry.chemical_classification, biology, Molecular Structure, Chemistry, Organic Chemistry, Enzyme, Enzyme inhibitor, biology.protein, Molecular Medicine, Ethylamine

Abstract

Inhibition of the aspartyl protease BACE-1 has the potential to deliver a disease-modifying therapy for Alzheimer’s disease. Herein, is described the lead generation effort which resulted, with the support of X-ray crystallography, in the discovery of potent inhibitors based on a hydroxy ethylamine (HEA) transition-state mimetic. These inhibitors were capable of lowering amyloid production in a cell-based assay.

Published

2007