Your search keyword '"Laurie J. Gordon"' showing total 40 results

1. Identification and Optimization of a Ligand-Efficient Benzoazepinone Bromodomain and Extra Terminal (BET) Family Acetyl-Lysine Mimetic into the Oral Candidate Quality Molecule I-BET432

Author

Philip G. Humphreys, Niall A. Anderson, Paul Bamborough, Andrew Baxter, Chun-wa Chung, Rosa Cookson, Peter D. Craggs, Toryn Dalton, Julie C. L. Fournier, Laurie J. Gordon, Heather F. Gray, Matthew W. Gray, Richard Gregory, David J. Hirst, Craig Jamieson, Katherine L. Jones, Hripsimee Kessedjian, David Lugo, Grant McGonagle, Vipulkumar K. Patel, Christopher Patten, Darren L. Poole, Rab K. Prinjha, Cesar Ramirez-Molina, Inmaculada Rioja, Gail Seal, Kayleigh A. J. Stafford, Rishi R. Shah, Daniel Tape, Natalie H. Theodoulou, Laura Tomlinson, Sabri Ukuser, Ian D. Wall, Natalie Wellaway, and Gemma White

Subjects

Histones, Protein Domains, Lysine, Drug Discovery, Humans, Molecular Medicine, Ligands, Transcription Factors

Abstract

The bromodomain and extra terminal (BET) family of proteins are an integral part of human epigenome regulation, the dysregulation of which is implicated in multiple oncology and inflammatory diseases. Disrupting the BET family bromodomain acetyl-lysine (KAc) histone protein-protein interaction with small-molecule KAc mimetics has proven to be a disease-relevant mechanism of action, and multiple molecules are currently undergoing oncology clinical trials. This work describes an efficiency analysis of published GSK pan-BET bromodomain inhibitors, which drove a strategic choice to focus on the identification of a ligand-efficient KAc mimetic with the hypothesis that lipophilic efficiency could be drastically improved during optimization. This focus drove the discovery of the highly ligand-efficient and structurally distinct benzoazepinone KAc mimetic. Following crystallography to identify suitable growth vectors, the benzoazepinone core was optimized through an explore-exploit structure-activity relationship (SAR) approach while carefully monitoring lipophilic efficiency to deliver I-BET432 (

Published

2022

2. Optimization of a Series of RIPK2 PROTACs

Author

Don T. Fisher, Gillian F. Watt, Ian Churcher, Laurie J. Gordon, Andrea D Gonçalves, Alina Mares, Phoebe Dace, Rakesh Nagilla, Bartholomew J. Votta, Ian Edward David Smith, John D. Harling, Pamela A. Haile, Afjal Hussain Miah, Paul Giffen, Paul Scott-Stevens, Aditya R. Thawani, Mark David Rackham, and Jane Denyer

Subjects

Male, Molecular Structure, THP-1 Cells, Kinase, Chemistry, Molecular Pharmacology, Pharmacology, Inhibitor of apoptosis, Rats, Rats, Sprague-Dawley, RIPK2, Serine, Gene Expression Regulation, Receptor-Interacting Protein Serine-Threonine Kinase 2, Drug Design, Drug Discovery, Lipophilicity, Animals, Humans, Molecular Medicine, Rats, Wistar, Threonine, Protein kinase A, Half-Life

Abstract

Receptor-interacting serine/threonine protein kinase 2 (RIPK2) is an important kinase of the innate immune system. Herein, we describe the optimization of a series of RIPK2 PROTACs which recruit members of the inhibitor of apoptosis (IAP) family of E3 ligases. Our PROTAC optimization strategy focused on reducing the lipophilicity of the early lead which resulted in the identification of analogues with improved solubility and increased human and rat microsomal stability. We identified a range of IAP binders that were successfully incorporated into potent RIPK2 PROTACs with attractive pharmacokinetic profiles. Compound 20 possessed the best overall profile with good solubility, potent degradation of RIPK2, and associated inhibition of TNFα release. A proof-of-concept study utilizing a slow release matrix demonstrated the feasibility of a long-acting parenteral formulation with >1 month duration. This represents an attractive alternative dosing paradigm to oral delivery, especially for chronic diseases where compliance can be challenging.

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. Development of an intracellular quantitative assay to measure compound binding kinetics

Author

Emma J. Jones, Charles S. Lay, Charlotte E. Carver, John P. Evans, Kristopher McCombe, Alexander N Phillipou, Daniel Thomas, Peter D. Craggs, Cassie Messenger, Mahnoor Mahmood, Kelly M Gatfield, Kristin M. Riching, Laurie J. Gordon, and Matthew Campbell

Subjects

Bioluminescence Resonance Energy Transfer Techniques, Clinical Biochemistry, Nerve Tissue Proteins, Receptors, Cell Surface, Biology, Biochemistry, law.invention, law, Drug Discovery, Humans, Luciferase, Luciferases, Molecular Biology, IC50, Cells, Cultured, Fluorescent Dyes, Pharmacology, Binding Sites, Drug discovery, Receptor–ligand kinetics, Bromodomain, Kinetics, HEK293 Cells, Biological target, Biophysics, Recombinant DNA, Molecular Medicine, Female, Intracellular

Abstract

Contemporary drug discovery typically quantifies the effect of a molecule on a biological target using the equilibrium-derived measurements of IC50, EC50, or KD. Kinetic descriptors of drug binding are frequently linked with the effectiveness of a molecule in modulating a disease phenotype; however, these parameters are yet to be fully adopted in early drug discovery. Nanoluciferase bioluminescence resonance energy transfer (NanoBRET) can be used to measure interactions between fluorophore-conjugated probes and luciferase fused target proteins. Here, we describe an intracellular NanoBRET competition assay that can be used to quantify cellular kinetic rates of compound binding to nanoluciferase-fused bromodomain and extra-terminal (BET) proteins. Comparative rates are generated using a cell-free NanoBRET assay and by utilizing orthogonal recombinant protein-based methodologies. A screen of known pan-BET inhibitors is used to demonstrate the value of this approach in the investigation of kinetic selectivity between closely related proteins.

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. Cellular Target Engagement Approaches to Monitor Epigenetic Reader Domain Interactions

Author

Cassie Messenger, Laurie J. Gordon, Simon C. C. Lucas, Aaron T. Cheng, Kelly M Gatfield, John P. Evans, Emma J. Jones, Mahnoor Mahmood, Charles S. Lay, Charlotte E. Carver, Douglas Sammon, Antonia J. Lewis, Alexander N Phillipou, Syandan Chakraborty, Luke A Greenhough, Peter D. Craggs, and David J Brierley

Subjects

BRD4, Computational biology, Biochemistry, Chromatin remodeling, Analytical Chemistry, Epigenesis, Genetic, 03 medical and health sciences, Structure-Activity Relationship, 0302 clinical medicine, Fluorescence Resonance Energy Transfer, Humans, Luciferase, Epigenetics, Luciferases, 030304 developmental biology, 0303 health sciences, biology, DNA Methylation, Chromatin Assembly and Disassembly, Phenotype, Bromodomain, Histone Code, Histone, 030220 oncology & carcinogenesis, DNA methylation, biology.protein, Molecular Medicine, Biological Assay, Biotechnology

Abstract

Malfunctions in the basic epigenetic mechanisms such as histone modifications, DNA methylation, and chromatin remodeling are implicated in a number of cancers and immunological and neurodegenerative conditions. Within GlaxoSmithKline (GSK) we have utilized a number of variations of the NanoBRET technology for the direct measurement of compound-target engagement within native cellular environments to drive high-throughput, routine structure-activity relationship (SAR) profiling across differing epigenetic targets. NanoBRET is a variation of the bioluminescence resonance energy transfer (BRET) methodology utilizing proteins of interest fused to either NanoLuc, a small, high-emission-intensity luciferase, or HaloTag, a modified dehalogenase enzyme that can be selectively labeled with a fluorophore. The combination of these two technologies has enabled the application of NanoBRET to biological systems such as epigenetic protein-protein interactions, which have previously been challenging. By synergizing target engagement assays with more complex primary cell phenotypic assays, we have been able to demonstrate compound-target selectivity profiles to enhance cellular potency and offset potential liability risks. Additionally, we have shown that in the absence of a robust, cell phenotypic assay, it is possible to utilize NanoBRET target engagement assays to aid chemistry in progressing at a higher scale than would have otherwise been achievable. The NanoBRET target engagement assays utilized have further shown an excellent correlation with more reductionist biochemical and biophysical assay systems, clearly demonstrating the possibility of using such assay systems at scale, in tandem with, or in preference to, lower-throughput cell phenotypic approaches.

Published

2019

14. 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

15. 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

16. Cell Penetrant Inhibitors of the KDM4 and KDM5 Families of Histone Lysine Demethylases. 2. Pyrido[3,4-d]pyrimidin-4(3H)-one Derivatives

Author

Rab K. Prinjha, Alex Preston, Inma Rioja, Roy Katso, Melanie Leveridge, Chun-wa Chung, Michael David Barker, Laurens Kruidenier, Gerard Joberty, Kevin Lee, Onkar M. P. Singh, Joanna Taylor, Matthew Campbell, Michelle Pemberton, Fiona Brown, Robert Eagle, Carl Haslam, David Matthew Wilson, Neil Stuart Garton, Tracy Jane Shipley, Colin J. Suckling, Philip G. Humphreys, Gerard Drewes, Laurie J. Gordon, Pamela Thomas, Jack A. Brown, Gail A. Seal, Thomas George Christopher Hayhow, and Susan Marie Westaway

Subjects

Models, Molecular, 0301 basic medicine, Jumonji Domain-Containing Histone Demethylases, Cell Membrane Permeability, Cell, Pyrimidinones, Crystallography, X-Ray, 01 natural sciences, Cell Line, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Drug Discovery, Gene expression, medicine, Humans, Structure–activity relationship, Epigenetics, Enzyme Inhibitors, Histone Demethylases, 010405 organic chemistry, Chemistry, Drug discovery, 0104 chemical sciences, Molecular Docking Simulation, 030104 developmental biology, medicine.anatomical_structure, Biochemistry, Cell culture, Molecular Medicine, Penetrant (biochemical)

Abstract

Following the discovery of cell penetrant pyridine-4-carboxylate inhibitors of the KDM4 (JMJD2) and KDM5 (JARID1) families of histone lysine demethylases (e.g., 1), further optimization led to the identification of non-carboxylate inhibitors derived from pyrido[3,4-d]pyrimidin-4(3H)-one. A number of exemplars such as compound 41 possess interesting activity profiles in KDM4C and KDM5C biochemical and target-specific, cellular mechanistic assays.

Published

2016

17. Discovery of I-BRD9, a selective cell active chemical probe for bromodomain containing protein 9 inhibition

Author

Laurie J. Gordon, Matthew J Lindon, Nicholas C. O. Tomkinson, Chun-wa Chung, Isabelle Becher, Judit Molnar, Ka Hing Che, Paola Grandi, Andrew J. Bannister, David H. Drewry, Rab K. Prinjha, Antje Dittmann, Tony Kouzarides, Natalie Hope Theodoulou, Rino A. Bit, Philip G. Humphreys, Anne-Marie Michon, Samuel Robson, Gerard Drewes, Melanie Leveridge, and Paul Bamborough

Subjects

Models, Molecular, 0301 basic medicine, Lysine, Crystallography, X-Ray, Article, Cell Line, Small Molecule Libraries, 03 medical and health sciences, Protein acylation, Transcription (biology), Drug Discovery, Humans, Amino Acid Sequence, Gene, Binding Sites, biology, Chemistry, Biomedical Sciences, Molecular biology, Bromodomain, Chromatin, Cell biology, Molecular Docking Simulation, QD450, 030104 developmental biology, Histone, Acetylation, biology.protein, Molecular Medicine, Transcription Factors

Abstract

Acetylation of histone lysine residues is one of the most well-studied post-translational modifications of chromatin, selectively recognized by bromodomain ‘reader’ modules. Inhibitors of the Bromodomain and Extra Terminal domain (BET) family of bromodomains have shown profound anti-cancer and anti-inflammatory properties, generating much interest in targeting other bromodomain-containing proteins for disease treatment. Herein, we report the discovery of I-BRD9, the first selective cellular chemical probe for Bromodomain-containing protein 9 (BRD9). I-BRD9 was identified through structure-based design, leading to greater than 700-fold selectivity over the BET family and 200-fold over the highly homologous Bromodomain-containing protein 7 (BRD7). I-BRD9 was used to identify genes regulated by BRD9 in Kasumi-1 cells involved in oncology and immune response pathways and to the best of our knowledge, represents the first selective tool compound available to elucidate the cellular phenotype of BRD9 bromodomain inhibition.

Published

2016

18. 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

19. The structure based design of dual HDAC/BET inhibitors as novel epigenetic probes

Author

Stephen John Atkinson, Chun-wa Chung, Peter Ernest Soden, Laurie J. Gordon, Rab K. Prinjha, Nicholas Smithers, Rebecca C. Furze, Kathryn A. Giblin, Davina C. Angell, Marcus Bantscheff, Nigel J. Parr, Inmaculada Rioja, Jason Witherington, and Gerard Drewes

Subjects

Pharmacology, Hydroxamic acid, Organic Chemistry, Pharmaceutical Science, hemic and immune systems, chemical and pharmacologic phenomena, Biology, Biochemistry, Small molecule, In vitro, Bromodomain, chemistry.chemical_compound, chemistry, Transcription (biology), Drug Discovery, Cancer cell, Molecular Medicine, Histone deacetylase, Epigenetics

Abstract

Herein we describe the design and synthesis of a dual active histone deacetylase (HDAC)/bromodomain and extra terminal (BET) small molecule tool inhibitor, DUAL946 (1). Exploiting our extensive epigenetic toolbox, we achieved the functionalisation of a BET active tetrahydroquinoline (THQ) core, with a hydroxamic acid HDAC inhibitor (HDACi) motif. Dual inhibition of BET and HDAC proteins was confirmed by in vitro biochemical and biophysical testing and through chemoproteomic competition experiments in cell lysates. This activity was translated into potent cellular activity in both immune and cancer cells.

Published

2014

20. Discovery of a Potent, Cell Penetrant, and Selective p300/CBP-Associated Factor (PCAF)/General Control Nonderepressible 5 (GCN5) Bromodomain Chemical Probe

Author

Laurie J. Gordon, Paola Grandi, Chun-wa Chung, Katherine Louise Jones, Colin J. Suckling, Jameed Hussain, Matthew J Lindon, David F. Tough, Philip G. Humphreys, Thomas George Christopher Hayhow, Jessica F. Renaux, Paul Bamborough, Peter D. Craggs, Rab K. Prinjha, and Anne-Marie Michon

Subjects

0301 basic medicine, Cell Membrane Permeability, Protein domain, Cell, 01 natural sciences, 03 medical and health sciences, Mice, Structure-Activity Relationship, Piperidines, Protein Domains, Transcription (biology), Drug Discovery, medicine, Structure–activity relationship, Animals, Humans, p300-CBP Transcription Factors, CREB-binding protein, Histone Acetyltransferases, biology, 010405 organic chemistry, Chemistry, Membranes, Artificial, Stereoisomerism, 0104 chemical sciences, Cell biology, Bromodomain, Pyridazines, enzymes and coenzymes (carbohydrates), 030104 developmental biology, medicine.anatomical_structure, PCAF, Biochemistry, Viral replication, Molecular Probes, biology.protein, Molecular Medicine

Abstract

p300/CREB binding protein associated factor (PCAF/KAT2B) and general control nonderepressible 5 (GCN5/KAT2A) are multidomain proteins that have been implicated in retroviral infection, inflammation pathways, and cancer development. However, outside of viral replication, little is known about the dependence of these effects on the C-terminal bromodomain. Herein, we report GSK4027 as a chemical probe for the PCAF/GCN5 bromodomain, together with GSK4028 as an enantiomeric negative control. The probe was optimized from a weakly potent, nonselective pyridazinone hit to deliver high potency for the PCAF/GCN5 bromodomain, high solubility, cellular target engagement, and ≥18000-fold selectivity over the BET family, together with ≥70-fold selectivity over the wider bromodomain families.

Published

2016

21. 8-Piperazinyl-2,3-dihydropyrrolo[3,2-g]isoquinolines: potent, selective, orally bioavailable 5-HT1 receptor ligands

Author

Neil Upton, Tania O. Stean, Claire Roberts, Michael S. Hadley, Vicky Holland, Gary W. Price, Laurie J. Gordon, Jeannette M. Watson, Jenifer Powles, Claire M. Scott, Leanne Cutler, Tanya Coleman, Tom D. Heightman, Andrew Ayrton, Jean-Pierre Pilleux, Sarah L. Pardoe, Graham J. Riley, Laramie Mary Gaster, Nigel E. Austin, Brenda K. Trail, and Derek N. Middlemiss

Subjects

Adrenergic receptor, Stereochemistry, medicine.drug_class, Clinical Biochemistry, Administration, Oral, Biological Availability, Pharmaceutical Science, Ligands, Biochemistry, Partial agonist, Structure-Activity Relationship, Dopamine, Drug Discovery, medicine, Animals, Receptor, Molecular Biology, 5-HT receptor, Brain Chemistry, Chemistry, Organic Chemistry, Isoquinolines, Receptor antagonist, Rats, Serotonin Receptor Agonists, Receptor, Serotonin, 5-HT1D, Receptors, Serotonin, Receptor, Serotonin, 5-HT1A, Receptor, Serotonin, 5-HT1B, Molecular Medicine, 5-HT1 receptor, Serotonin Antagonists, Serotonin, medicine.drug

Abstract

The novel 8-piperazinyl-2,3-dihydropyrroloisoquinoline template was synthesized in nine steps. The template was N-substituted to give a series of compounds showing binding to human cloned 5-HT1A, 5-HT1B and 5-HT1D receptors with pKi’s greater than 9 and selectivities up to 1000-fold against other serotonin, dopamine and adrenergic receptors. Several compounds were shown to possess weak partial agonist activity in cloned receptors, which translated to antagonism in in vitro studies.

Published

2016

22. Fragment-Based Discovery of Bromodomain Inhibitors Part 2: Optimization of Phenylisoxazole Sulfonamides

Author

Jonathan Thomas Seal, Jonathan D. Goodacre, Chun-wa Chung, Laurie J. Gordon, Antonia J. Lewis, Paul Bamborough, David Matthew Wilson, Hawa Diallo, and Woodrow Michael David

Subjects

Models, Molecular, Cell Cycle Proteins, Fluorescence Polarization, Protein Serine-Threonine Kinases, Crystallography, X-Ray, Structure-Activity Relationship, chemistry.chemical_compound, Fragment (logic), Histone tails, Signaling proteins, Drug Discovery, Humans, Epigenetics, Isoxazole, chemistry.chemical_classification, Sulfonamides, Molecular Structure, Anti-Inflammatory Agents, Non-Steroidal, Nuclear Proteins, Isoxazoles, Surface Plasmon Resonance, Sulfonamide, Bromodomain, Solubility, chemistry, Biochemistry, Leukocytes, Mononuclear, Cytokines, Molecular Medicine, Protein Binding, Transcription Factors

Abstract

Bromodomains are epigenetic reader modules that regulate gene transcription through their recognition of acetyl-lysine modified histone tails. Inhibitors of this protein-protein interaction have the potential to modulate multiple diseases as demonstrated by the profound anti-inflammatory and antiproliferative effects of a recently disclosed class of BET compounds. While these compounds were discovered using phenotypic assays, here we present a highly efficient alternative approach to find new chemical templates, exploiting the abundant structural knowledge that exists for this target class. A phenyl dimethyl isoxazole chemotype resulting from a focused fragment screen has been rapidly optimized through structure-based design, leading to a sulfonamide series showing anti-inflammatory activity in cellular assays. This proof-of-principle experiment demonstrates the tractability of the BET family and bromodomain target class to fragment-based hit discovery and structure-based lead optimization.

Published

2012

23. Configuration of a High-Content Imaging Platform for Hit Identification and Pharmacological Assessment of JMJD3 Demethylase Enzyme Inhibitors

Author

Angela Bridges, Bhumika Karamshi, Roy Katso, Laurie J. Gordon, Kirsty Gill, Alpa Mulji, Laurens Kruidenier, Emma J. Jones, Julia Smith, Robert Tanner, Fiona Brown, Mike D. Barker, Joanna Taylor, Arshad Sheikh, Sue Hutchinson, Rob Jepras, Rebecca Randle, Mike Woodrow, Melanie Leveridge, Murray J. B. Brown, John Liddle, Jordi Munoz-Muriedas, Penny A. Smee, Robert Eagle, Carl Haslam, Margaret Martin, and Pamela Thomas

Subjects

Jumonji Domain-Containing Histone Demethylases, Population, Computational biology, Biology, Biochemistry, Cellular viability, Permeability, Cell Line, Analytical Chemistry, Histones, Small Molecule Libraries, Antibody Specificity, Statistical analyses, Image Processing, Computer-Assisted, Humans, Enzyme Inhibitors, education, chemistry.chemical_classification, Genetics, education.field_of_study, Lysine, Cellular imaging, Reproducibility of Results, Recombinant Proteins, High-Throughput Screening Assays, Enzyme, chemistry, biology.protein, Molecular Medicine, Demethylase, Identification (biology), Histone Demethylases, Biotechnology

Abstract

The biological complexity associated with the regulation of histone demethylases makes it desirable to configure a cellular mechanistic assay format that simultaneously encompasses as many of the relevant cellular processes as possible. In this report, the authors describe the configuration of a JMJD3 high-content cellular mechanistic imaging assay that uses single-cell multiparameter measurements to accurately assess cellular viability and the enzyme-dependent demethylation of the H3K27(Me)3 mark by exogenously expressed JMJD3. This approach couples robust statistical analyses with the spatial resolving power of cellular imaging. This enables segregation of expressing and nonexpressing cells into discrete subpopulations and consequently pharmacological quantification of compounds of interest in the expressing population at varying JMJD3 expression levels. Moreover, the authors demonstrate the utility of this hit identification strategy through the successful prosecution of a medium-throughput focused campaign of an 87 500-compound file, which has enabled the identification of JMJD3 cellular-active chemotypes. This study represents the first report of a demethylase high-content imaging assay with the ability to capture a repertoire of pharmacological tools, which are likely both to inform our mechanistic understanding of how JMJD3 is modulated and, more important, to contribute to the identification of novel therapeutic modalities for this demethylase enzyme.

Published

2012

24. Acylglycinamides as inhibitors of glycine transporter type 1

Author

Laurie J. Gordon, Gemma V. Puckey, Wyman Paul Adrian, David John Nash, Richard Blunt, Hugh J. Herdon, Simon Teague, Victoria Hadden, Stefano Fontana, Amanda Johns, and Roderick A. Porter

Subjects

Stereochemistry, Clinical Biochemistry, Glycine, Pharmaceutical Science, Glycine Plasma Membrane Transport Proteins, Biochemistry, Glycine transporter, Inhibitory Concentration 50, Structure-Activity Relationship, Drug Discovery, Animals, Humans, Structure–activity relationship, Solubility, Molecular Biology, Chemistry, Organic Chemistry, Combinatorial chemistry, Rats, Bioavailability, Lipophilicity, Molecular Medicine, Selectivity

Abstract

A screening hit was used as the basis for the core structure of a new series of acylglycinamide GlyT-1 inhibitors. Investigation of the SAR around four areas of diversity used facile chemistry to prepare compounds quickly. By focussing on reducing the lipophilicity and improving the aqueous solubility in the series we were able to prepare a compound (17e) with a good level of activity at GlyT-1, selectivity over GlyT-2 and moderate oral bioavailability.

Published

2011

25. 5-{2-[4-(2-Methyl-5-quinolinyl)-1-piperazinyl]ethyl}-2(1H)-quinolinones and 3,4-dihydro-2(1H)-quinolinones: Dual-acting 5-HT1 receptor antagonists and serotonin reuptake inhibitors. Part 3

Author

Laurie J. Gordon, Anna-Maria Capelli, Laura Zonzini, Manuela Borriello, Romano Di-Fabio, Enrica Granci, Massimo Gianotti, Roberto Arban, Simone Spada, Barbara Bertani, Stefania Faedo, Valeria Zucchelli, Alessandra Pasquarello, Angela Worby, and Steven Mark Bromidge

Subjects

Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Quinolones, Pharmacology, Biochemistry, Chemical synthesis, Drug Discovery, Animals, Molecular Biology, 5-HT receptor, Serotonin transporter, Autoreceptors, biology, Chemistry, Organic Chemistry, Antagonist, Rats, Synapses, Autoreceptor, biology.protein, Molecular Medicine, 5-HT1 receptor, Serotonin, Reuptake inhibitor, Receptors, Serotonin, 5-HT1, Selective Serotonin Reuptake Inhibitors

Abstract

5-{2-[4-(2-Methyl-5-quinolinyl)-1-piperazinyl]ethyl}-2(1H)-quinolinones and 3,4-dihydro-2(1H)-quinolinones have been identified with different combinations of 5-HT(1) autoreceptor antagonist and hSerT potencies and excellent rat PK profiles. The availability of tool compounds with a range of profiles at targets known to play a key role in the control of synaptic 5-HT levels will allow exploration of different pharmacological profiles in a range of animal behavioral and disease models.

Published

2010

26. Design and Synthesis of Novel Tricyclic Benzoxazines as Potent 5-HT1A/B/D Receptor Antagonists Leading to the Discovery of 6-{2-[4-(2-methyl-5-quinolinyl)-1-piperazinyl]ethyl}-4H-imidazo[5,1-c][1,4]benzoxazine-3-carboxamide (GSK588045)

Author

Ilaria Sartori, Laura Zonzini, Laurie J. Gordon, Angela Worby, Stefano Fontana, Manuela Borriello, Silvia Bison, Jeannette M. Watson, Steven Mark Bromidge, Giovanna Dal Forno, Colin Philip Leslie, Alessandra Pasquarello, Anna Sava, Luca G. Moccia, Barbara Bertani, Roberto Arban, Daniele Donati, Enrica Granci, Valeria Zucchelli, Paolo Cavanni, Massimo Gianotti, and Romano Di-Fabio

Subjects

chemistry.chemical_classification, biology, medicine.drug_class, Stereochemistry, Benzoxazinones, hERG, Carboxamide, Receptor antagonist, chemistry, In vivo, Drug Discovery, medicine, biology.protein, Molecular Medicine, Receptor, Serotonin transporter, Tricyclic

Abstract

Bioisoteric replacement of the metabolically labile N-methyl amide group of a series of benzoxazinones with small heterocyclic rings has led to novel series of fused tricyclic benzoxazines which are potent 5-HT1A/B/D receptor antagonists with and without concomitant human serotonin transporter (hSerT) activity. Optimizing against multiple parameters in parallel identified 6-{2-[4-(2-methyl-5-quinolinyl)-1-piperazinyl]ethyl}-4H-imidazo[5,1-c][1,4]benzoxazine-3-carboxamide (GSK588045) as a potent 5-HT1A/B/D receptor antagonist with a high degree of selectivity over human ether-a-go-go related gene (hERG) potassium channels, favorable pharmacokinetics, and excellent activity in vivo in rodent pharmacodynamic (PD) models. On the basis of its outstanding overall profile, this compound was progressed as a clinical candidate with the ultimate aim to assess its potential as a faster acting antidepressant/anxiolytic with reduced side-effect burden.

Published

2010

27. 8-[2-(4-Aryl-1-piperazinyl)ethyl]-2H-1,4-benzoxazin-3(4H)-ones: Dual-acting 5-HT1 receptor antagonists and serotonin reuptake inhibitors—Part II

Author

Steven M, Bromidge, Barbara, Bertani, Manuela, Borriello, Andrea, Bozzoli, Stefania, Faedo, Massimo, Gianotti, Laurie J, Gordon, Matthew, Hill, Valeria, Zucchelli, Jeannette M, Watson, and Laura, Zonzini

Subjects

ERG1 Potassium Channel, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, CHO Cells, Serotonin 5-HT1 Receptor Antagonists, Biochemistry, Ether-A-Go-Go Potassium Channels, Piperazines, Benzoxazines, Rats, Cricetulus, Cricetinae, Drug Discovery, Animals, Humans, Molecular Medicine, Serotonin Antagonists, Receptors, Serotonin, 5-HT1, Molecular Biology, Selective Serotonin Reuptake Inhibitors

Abstract

8-[2-(4-Aryl-1-piperazinyl)ethyl]-2H-1,4-benzoxazin-3(4H)-ones have been identified as highly potent 5-HT(1A/B/D) receptor antagonists with and without additional SerT activity and a high degree of selectivity over hERG potassium channels. Modulation of the different target activities gave compounds with a range of profiles suitable for further in vivo characterization.

Published

2009

28. 6-[2-(4-Aryl-1-piperazinyl)ethyl]-2H-1,4-benzoxazin-3(4H)-ones: Dual-acting 5-HT1 receptor antagonists and serotonin reuptake inhibitors

Author

Alessia Vesentini, Luigi Piero Stasi, Barbara Bertani, Matthew Hill, Jeannette M. Watson, Steven Mark Bromidge, Enrica Granci, Laura Zonzini, Valeria Zucchelli, Howard Robert Marshall, Stefania Faedo, Giancarlo Merlo, Laurie J. Gordon, and Manuela Borriello

Subjects

Tertiary amine, Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Serotonin 5-HT1 Receptor Antagonists, Biochemistry, Piperazines, Drug Discovery, Animals, Humans, Receptor, Piperazine, Molecular Biology, 5-HT receptor, Benzoxazoles, Bicyclic molecule, Chemistry, Organic Chemistry, Antidepressive Agents, Rats, Liver, Models, Chemical, Drug Design, Molecular Medicine, Antidepressant, 5-HT1 receptor, Serotonin Antagonists, Serotonin, Reuptake inhibitor, Selective Serotonin Reuptake Inhibitors

Abstract

Investigation of a series 6-[2-(4-aryl-1-piperazinyl)ethyl]-2H-1,4-benzoxazin-3(4H)-ones has led to the discovery of potent 5-HT(1A/1B/1D) receptor antagonists with and without additional SerT affinity. Modulation of the different target activities gave compounds with a range of profiles suitable for further in vivo characterization.

Published

2008

29. Cell Penetrant Inhibitors of the KDM4 and KDM5 Families of Histone Lysine Demethylases. 1. 3-Amino-4-pyridine Carboxylate Derivatives

Author

Laurens Kruidenier, Rebecca Randle, Hawa Diallo, Inma Rioja, Clement Douault, Anne Rueger, Chun-wa Chung, Thomas George Christopher Hayhow, Rab K. Prinjha, Alex Preston, Roy Katso, Matthew Campbell, Michael David Barker, J. Mosley, Kevin Lee, Joanna Taylor, Marcel Muelbaier, Douglas W. Thomson, Gail A. Seal, Jack A. Brown, Susan Marie Westaway, Onkar M. P. Singh, Gerard Joberty, Philip G. Humphreys, Melanie Leveridge, Laurie J. Gordon, Pamela Thomas, Carl Haslam, Fiona Brown, John Liddle, Gerard Drewes, Robert Eagle, Robert J. Sheppard, and David Matthew Wilson

Subjects

0301 basic medicine, Models, Molecular, Jumonji Domain-Containing Histone Demethylases, Cell Membrane Permeability, Pyridines, Cell, Crystallography, X-Ray, 01 natural sciences, Cell Line, 03 medical and health sciences, Oxidoreductase, Transcription (biology), Drug Discovery, medicine, Humans, Enzyme Inhibitors, IC50, Amination, chemistry.chemical_classification, Histone Demethylases, 010405 organic chemistry, 0104 chemical sciences, 030104 developmental biology, medicine.anatomical_structure, chemistry, Biochemistry, Cell culture, Drug Design, Molecular Medicine, Selectivity

Abstract

Optimization of KDM6B (JMJD3) HTS hit 12 led to the identification of 3-((furan-2-ylmethyl)amino)pyridine-4-carboxylic acid 34 and 3-(((3-methylthiophen-2-yl)methyl)amino)pyridine-4-carboxylic acid 39 that are inhibitors of the KDM4 (JMJD2) family of histone lysine demethylases. Compounds 34 and 39 possess activity, IC50 ≤ 100 nM, in KDM4 family biochemical (RFMS) assays with ≥ 50-fold selectivity against KDM6B and activity in a mechanistic KDM4C cell imaging assay (IC50 = 6-8 μM). Compounds 34 and 39 are also potent inhibitors of KDM5C (JARID1C) (RFMS IC50 = 100-125 nM).

Published

2016

30. Direct Measurement of Intracellular Compound Concentration by RapidFire Mass Spectrometry Offers Insights into Cell Permeability

Author

Laurie J. Gordon, Andrew West, André Mateus, Michael M. Hann, Klára Valkó, Bill Leavens, Simon A. Readshaw, Morven Allen, Per Artursson, and Gareth Wayne

Subjects

0301 basic medicine, Synthetic membrane, Pharmacology, Mass spectrometry, Tandem mass spectrometry, Biochemistry, Permeability, Analytical Chemistry, HeLa, 03 medical and health sciences, Liquid chromatography–mass spectrometry, Tandem Mass Spectrometry, Cell Line, Tumor, Drug Discovery, Humans, Cell permeability, Chromatography, biology, Drug discovery, biology.organism_classification, High-Throughput Screening Assays, 030104 developmental biology, Pharmaceutical Preparations, Molecular Medicine, Intracellular, Biotechnology, Chromatography, Liquid, HeLa Cells

Abstract

One of the key challenges facing early stage drug discovery is understanding the commonly observed difference between the activity of compounds in biochemical assays and cellular assays. Traditionally, indirect or estimated cell permeability measurements such as estimations from logP or artificial membrane permeability are used to explain the differences. The missing link is a direct measurement of intracellular compound concentration in whole cells. This can, in some circumstances, be estimated from the cellular activity, but this may also be problematic if cellular activity is weak or absent. Advances in sensitivity and throughput of analytical techniques have enabled us to develop a high-throughput assay for the measurement of intracellular compound concentration for routine use to support lead optimization. The assay uses a RapidFire-MS based readout of compound concentration in HeLa cells following incubation of cells with test compound. The initial assay validation was performed by ultra-high performance liquid chromatography tandem mass spectrometry, and the assay was subsequently transferred to RapidFire tandem mass spectrometry. Further miniaturization and optimization were performed to streamline the process, increase sample throughput, and reduce cycle time. This optimization has delivered a semi-automated platform with the potential of production scale compound profiling up to 100 compounds per day.

Published

2015

31. Pharmacological Profile of Antipsychotics at Monoamine Receptors: Atypicality Beyond 5-HT2A Receptor Blockade

Author

Andrew D. Gribble, Laurie J. Gordon, Claire M. Scott, Ceri H. Davies, Angela Worby, Jennie Heath, Martyn D. Wood, Kirsten L. Clarke, Katherine J. Cato, Graham J. Riley, Lorraine Campbell, Declan N.C. Jones, and Nisha Patel

Subjects

Dibenzothiazepines, Serotonin, medicine.medical_specialty, Dopamine, medicine.medical_treatment, CHO Cells, Serotonin 5-HT1 Receptor Antagonists, Pharmacology, Binding, Competitive, Synaptic Transmission, Partial agonist, Piperazines, Receptors, Dopamine, Benzodiazepines, Quetiapine Fumarate, Cricetinae, Dopamine receptor D2, Internal medicine, Receptor, Serotonin, 5-HT2C, medicine, Animals, Humans, Biogenic Monoamines, Receptor, Serotonin, 5-HT2A, Ziprasidone, Antipsychotic, Receptor, Clozapine, musculoskeletal, neural, and ocular physiology, General Neuroscience, Serotonin 5-HT1 Receptor Agonists, Serotonin Receptor Agonists, Thiazoles, Monoamine neurotransmitter, Endocrinology, Olanzapine, Receptors, Serotonin, Receptor, Serotonin, 5-HT1A, Schizophrenia, Serotonin 5-HT2 Receptor Antagonists, cardiovascular system, Aripiprazole, Serotonin Antagonists, Psychology, Antipsychotic Agents, medicine.drug

Abstract

Antipsychotic drugs (APD) are widely prescribed for the treatment of schizophrenia. The APD are differentiated into typical and atypical based on the lower incidence of extra-pyramidal side-effects associated with the newer atypical APD. It was suggested that atypicality may arise from an interaction with the 5-hydroxytryptamine (5-HT)(2) receptor and specifically on the 5-HT(2):dopamine D(2) affinity ratio. It is now realised that multiple subtypes of these receptors exist and that in addition, atypical APD interact with many monoamine receptors. The aim of the present study was to characterise the interaction of APD with a variety of monoamine receptors in terms of both affinity and efficacy. The data produced has highlighted that the atypical profile of APD such as olanzapine and clozapine may reflect antagonism of the 5-HT(2A) and 5-HT(2C) receptors, whilst that of, ziprasidone and quetiapine may reflect partial agonist activity at the 5-HT(1A) receptor, and that of aripiprazole may reflect partial agonist activity at the 5-HT(1A) receptor as well as is its claimed partial agonist activity at the dopamine D(2) receptor.

Published

2006

32. SB-649915, a novel, potent 5-HT1A and 5-HT1B autoreceptor antagonist and 5-HT re-uptake inhibitor in native tissue

Author

Christopher N. Johnson, Gary W. Price, Jeannette M. Watson, Ellen M. Soffin, Laurie J. Gordon, Claire M. Scott, Christopher J. Langmead, Paul Bryan Wren, Stefania Faedo, James J. Hagan, Matthew Hill, Steve M. Bromidge, and Peter J. Atkinson

Subjects

Agonist, Serotonin, Intrinsic activity, medicine.drug_class, Guinea Pigs, Stimulation, In Vitro Techniques, Serotonin 5-HT1 Receptor Antagonists, Biology, Pharmacology, Binding, Competitive, Rats, Sprague-Dawley, Mice, Radioligand Assay, Piperidines, medicine, Animals, Humans, Receptor, 5-HT receptor, Autoreceptors, Cerebral Cortex, Dose-Response Relationship, Drug, Callithrix, Serotonin 5-HT1 Receptor Agonists, Recombinant Proteins, Benzoxazines, Rats, Serotonin Receptor Agonists, Mechanism of action, Guanosine 5'-O-(3-Thiotriphosphate), Receptor, Serotonin, 5-HT1D, Receptor, Serotonin, 5-HT1A, Quinolines, Receptor, Serotonin, 5-HT1B, Autoreceptor, Raphe Nuclei, 5-HT1A receptor, Serotonin Antagonists, medicine.symptom, Selective Serotonin Reuptake Inhibitors

Abstract

An increase in brain 5-HT levels is thought to be the key mechanism of action which results in an antidepressant response. It has been proven that selective serotonin re-uptake inhibitors are effective antidepressants but the delay to therapeutic onset of these agents is thought to be due to the time required for 5-HT1A, and possibly 5-HT1B, autoreceptor desensitisation. Therefore an agent incorporating 5-HT re-uptake inhibition coupled with 5-HT1A and/or 5-HT1B autoreceptor antagonism may provide a fast acting clinical agent. The current studies describe the in vitro profile of SB-649915 (6-[(1-{2-[(2-methylquinolin-5-yl)oxy]ethyl}piperidin-4-yl)methyl]-2H-1,4-benzoxazin-3(4H)-one), a novel compound which has high affinity for human recombinant 5-HT1A, 5-HT1B and 5-HT1D receptors (pKi values of 8.6, 8.0, 8.8, respectively) and the human recombinant 5-HT transporter (pKi value of 9.3). SB-649915 also displays high affinity for rat, guinea pig, mouse and marmoset native tissue 5-HT1A, 5-HT1B and 5-HT1D receptors and rat native tissue 5-HT transporters (pKi valuesor=7.5). In functional [35S]GTPgammaS binding studies, SB-649915 (up to 1 microM) does not display intrinsic activity in HEK293 cells expressing human recombinant 5-HT1A receptors but acts as a partial agonist at human recombinant 5-HT1B and 5-HT1D receptors with intrinsic activity values of 0.3 and 0.7, respectively, as compared to the full agonist 5-HT. From Schild analysis, SB-649915 caused a concentration-dependent, rightward shift of 5-HT-induced stimulation of basal [35S]GTPgammaS binding in cells expressing human recombinant 5-HT1A or 5-HT1B receptors to yield pA2 values of 9.0 and 7.9, respectively. In electrophysiological studies in rat dorsal raphe nucleus, SB-649915 did not affect the cell firing rate up to 1 microM but attenuated (+)8-hydroxy-2-(di-n-propylamino) tetralin-induced inhibition of cell firing with an apparent pKb value of 9.5. SB-649915 (1 microM) significantly attenuated exogenous 5-HT-induced inhibition of electrically-stimulated [3H]5-HT release from guinea pig cortex. In studies designed to enhance endogenous 5-HT levels, and therefore increase tone at 5-HT1B autoreceptors, SB-649915 significantly potentiated [3H]5-HT release at 100 and 1000 nM. In LLCPK cells expressing human recombinant 5-HT transporters and in rat cortical synaptosomes, SB-649915 inhibited [3H]5-HT re-uptake with pIC50 values of 7.9 and 9.7, respectively. In summary, SB-649915 is a novel, potent 5-HT1A/1B autoreceptor antagonist and 5-HT re-uptake inhibitor in native tissue systems and represents a novel mechanism that could offer fast acting antidepressant action.

Published

2006

33. Bicyclic heteroarylpiperazines as selective brain penetrant 5-HT6 receptor antagonists

Author

Jenifer Powles, Neil Upton, Kim Winborn, Nigel Deeks, Christopher N. Johnson, Tania Buck, Mahmood Ahmed, Brenda K. Trail, Darren Jason Mitchell, Mervyn Thompson, Vicky Holland, Laurie J. Gordon, Michael A. Briggs, Jon T. Seal, Stephen Moss, Ashley Garner, David R. Witty, Steven Mark Bromidge, Lorraine Campbell, Andrew D. Medhurst, Tania O. Stean, Geoffrey Stemp, and Dieter Hamprecht

Subjects

medicine.drug_class, Clinical Biochemistry, Molecular Conformation, Administration, Oral, Biological Availability, Pharmaceutical Science, Pharmacology, Blood–brain barrier, Biochemistry, Permeability, Piperazines, Structure-Activity Relationship, chemistry.chemical_compound, Dogs, Drug Discovery, medicine, Animals, Receptor, Molecular Biology, Bicyclic molecule, Organic Chemistry, Antagonist, Brain, Penetration (firestop), Receptor antagonist, Rats, medicine.anatomical_structure, chemistry, Blood-Brain Barrier, Receptors, Serotonin, 5-HT6 receptor, Molecular Medicine, Serotonin Antagonists, Penetrant (biochemical)

Abstract

Starting from the potent and selective but poorly brain penetrant 5-HT6 receptor antagonist SB-271046, a successful strategy for improving brain penetration was adopted involving conformational constraint with concomitant reduction in hydrogen bond count. This provided a series of bicyclic heteroarylpiperazines with high 5-HT6 receptor affinity. 5-Chloroindole 699929 combined high 5-HT6 receptor affinity with excellent brain penetration and also had good oral bioavailability in both rat and dog.

Published

2005

34. Discovery of the First Potent, Selective 5-Hydroxytryptamine1D Receptor Antagonist

Author

Claire M. Scott, Harrington Frank Peter, Susanna C. Hopley, Laurie J. Gordon, Simon E. Ward, and Jeannette M. Watson

Subjects

CHO Cells, In Vitro Techniques, Serotonin 5-HT1 Receptor Antagonists, Pharmacology, Binding, Competitive, Piperazines, Radioligand Assay, Structure-Activity Relationship, Cricetulus, Cricetinae, Drug Discovery, Animals, Selective receptor modulator, Receptor, Cerebral Cortex, Chemistry, Antagonist, Serotonin 5-HT1 Receptor Agonists, Serotonin reuptake, In vitro, Rats, Biochemistry, Quinolines, Molecular Medicine, 5-HT1D receptor, Selective Serotonin Reuptake Inhibitors

Abstract

A series of 5-(piperidinylethyloxy)quinoline 5-hydroxytryptamine(1D) (5-HT(1D)) receptor antagonists have been discovered from elaboration of the series of dual 5-hydroxytryptamine(1)-selective serotonin reuptake inhibitors (5HT(1)-SSRIs) reported previously. This is the first report of highly potent, selective antagonists for the 5-HT(1D) receptor, which represents an extremely useful set of pharmacological tools for further understanding the roles of the 5-HT(1) receptor subtypes.

Published

2005

35. Identification of a novel series of BET family bromodomain inhibitors: binding mode and profile of I-BET151 (GSK1210151A)

Author

Anne Marie Jeanne Bouillot, Frédéric Donche, Olivier Mirguet, Rab K. Prinjha, Gael Krysa, Edwige Nicodeme, Ann Louise Walker, Chun-wa Chung, Laurie J. Gordon, Kevin Lee, Soren Beinke, David Matthew Wilson, Inma Rioja, Toni Lewis, Leanne Cutler, Dave Lugo, Jonathan Thomas Seal, Jason Witherington, Paul Bamborough, Yann Lamotte, Scott McCleary, Jorge Kirilovsky, and Françoise Gellibert

Subjects

Models, Molecular, Clinical Biochemistry, Guinea Pigs, Pharmaceutical Science, Nerve Tissue Proteins, Plasma protein binding, Crystallography, X-Ray, Biochemistry, Heterocyclic Compounds, 4 or More Rings, chemistry.chemical_compound, Mice, In vivo, Signaling proteins, Drug Discovery, Animals, Binding site, Isoxazole, Molecular Biology, Inflammation, Binding Sites, Organic Chemistry, Quinoline, Isoxazoles, Bromodomain, Rats, chemistry, Quinolines, Molecular Medicine, Protein Binding

Abstract

A novel series of quinoline isoxazole BET family bromodomain inhibitors are discussed. Crystallography is used to illustrate binding modes and rationalize their SAR. One member, I-BET151 (GSK1210151A), shows good oral bioavailability in both the rat and minipig as well as demonstrating efficient suppression of bacterial induced inflammation and sepsis in a murine in vivo endotoxaemia model.

Published

2012

36. In vitro and in vivo characterization of the novel GABAB receptor positive allosteric modulator, 2-{1-[2-(4-chlorophenyl)-5-methylpyrazolo[1,5-a]pyrimidin-7-yl]-2-piperidinyl}ethanol (CMPPE)

Author

M. H. Selina Mok, Laura Zonzini, Laurie J. Gordon, Vivian J A Costantini, Massimo Gianotti, Enzo Valerio, Magalie Rocheville, Corrado Carignani, Elisabetta Perdona, Mauro Corsi, Prisca Martinelli, Filippo Visentini, Anna Maria Capelli, and Michela Tessari

Subjects

Agonist, Male, Baclofen, Allosteric modulator, Animal food, medicine.drug_class, Allosteric regulation, Drug Evaluation, Preclinical, CHO Cells, Cyclopentanes, Pharmacology, GABAB receptor, Motor Activity, Transfection, Hippocampus, Rats, Sprague-Dawley, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Eating, Radioligand Assay, Cricetinae, medicine, Animals, Humans, G protein-coupled inwardly-rectifying potassium channel, Molecular Targeted Therapy, Receptor, gamma-Aminobutyric Acid, Cerebral Cortex, Neurons, Brain, Membrane Proteins, Electrophysiological Phenomena, Rats, Pyrimidines, nervous system, chemistry, Receptors, GABA-B, GABA-B Receptor Agonists, Pyrazoles

Abstract

There is preclinical evidence supporting the finding that the GABA(B) receptor orthosteric agonist, baclofen, has significant effects on eating behavior suggesting the potential therapeutic application of this compound for the treatment of eating related disorders. However, the wide clinical use of baclofen might be limited by the appearance of sedative and motor impairment effects. The identification of positive allosteric modulators (PAMs) of GABA(B) receptors represents a novel therapeutic approach to reduce the centrally-mediated adverse effects typical of the GABA(B) receptor orthosteric agonist. In the present work, we report the in vitro profile of a novel chemical structure, 2-{1-[2-(4-chlorophenyl)-5-methylpyrazolo[1,5-a]pyrimidin-7-yl]-2-piperidinyl}ethanol (CMPPE) identified by screening the GSK compound collection. CMPPE potentiates GABA-stimulated [(35)S]GTPγS binding to membranes of human recombinant cell line and of rat brain cortex. GABA concentration-response curves (CRC) in the presence of fixed concentrations of CMPPE, in rat native tissue, revealed an increase of both the potency and maximal efficacy of GABA. A similar modulatory effect was observed in GABA(B) receptor-mediated activation of inwardly rectifying potassium channels in hippocampal neurons. CMPPE (30-100 mg/kg) and GS39783 (100 mg/kg) significantly decreased food consumption in rat without impairment on the animal locomotor activity. On the contrary, baclofen (2.5 mg/kg) decreased both food intake and motor performance. All together these findings confirm the role of GABA(B) system in controlling animal food intake and for the first time demonstrate that GABA(B) receptor PAMs may represent a novel pharmacological approach to treat eating disorders without unwanted sedative effects.

Published

2010

37. Design and synthesis of novel tricyclic benzoxazines as potent 5-HT(1A/B/D) receptor antagonists leading to the discovery of 6-{2-[4-(2-methyl-5-quinolinyl)-1-piperazinyl]ethyl}-4H-imidazo[5,1-c][1,4]benzoxazine-3-carboxamide (GSK588045)

Author

Steven M, Bromidge, Roberto, Arban, Barbara, Bertani, Silvia, Bison, Manuela, Borriello, Paolo, Cavanni, Giovanna, Dal Forno, Romano, Di-Fabio, Daniele, Donati, Stefano, Fontana, Massimo, Gianotti, Laurie J, Gordon, Enrica, Granci, Colin P, Leslie, Luca, Moccia, Alessandra, Pasquarello, Ilaria, Sartori, Anna, Sava, Jeannette M, Watson, Angela, Worby, Laura, Zonzini, and Valeria, Zucchelli

Subjects

Cerebral Cortex, Male, Serotonin Plasma Membrane Transport Proteins, ERG1 Potassium Channel, Guinea Pigs, Callithrix, In Vitro Techniques, Serotonin 5-HT1 Receptor Antagonists, Antidepressive Agents, Ether-A-Go-Go Potassium Channels, Benzoxazines, Cell Line, Rats, Rats, Sprague-Dawley, Radioligand Assay, Structure-Activity Relationship, Cricetulus, Anti-Anxiety Agents, Cytochrome P-450 Enzyme System, Cricetinae, Microsomes, Liver, Animals, Humans, Protein Binding

Abstract

Bioisoteric replacement of the metabolically labile N-methyl amide group of a series of benzoxazinones with small heterocyclic rings has led to novel series of fused tricyclic benzoxazines which are potent 5-HT(1A/B/D) receptor antagonists with and without concomitant human serotonin transporter (hSerT) activity. Optimizing against multiple parameters in parallel identified 6-{2-[4-(2-methyl-5-quinolinyl)-1-piperazinyl]ethyl}-4H-imidazo[5,1-c][1,4]benzoxazine-3-carboxamide (GSK588045) as a potent 5-HT(1A/B/D) receptor antagonist with a high degree of selectivity over human ether-a-go-go related gene (hERG) potassium channels, favorable pharmacokinetics, and excellent activity in vivo in rodent pharmacodynamic (PD) models. On the basis of its outstanding overall profile, this compound was progressed as a clinical candidate with the ultimate aim to assess its potential as a faster acting antidepressant/anxiolytic with reduced side-effect burden.

Published

2010

38. Studies on a series of potent, orally bioavailable, 5-HT(1) receptor ligands--part II

Author

Laurie J. Gordon, Sean Thomas Flynn, Simon E. Ward, Wyman Paul Adrian, Claire M. Scott, Susan H. Moore, Kevin M. Thewlis, Peter J. Lovell, Peter Eddershaw, and Paul W. Smith

Subjects

Clinical Biochemistry, Pharmaceutical Science, Administration, Oral, Biological Availability, Ligands, Biochemistry, chemistry.chemical_compound, Structure-Activity Relationship, Pharmacokinetics, Drug Discovery, Animals, heterocyclic compounds, Receptor, Molecular Biology, Serotonin transporter, biology, musculoskeletal, neural, and ocular physiology, Organic Chemistry, Quinoline, In vitro, Bioavailability, Rats, nervous system, chemistry, biology.protein, Quinolines, Molecular Medicine, 5-HT1 receptor, Selectivity, Receptors, Serotonin, 5-HT1

Abstract

A series of 5-(piperidinylethyloxy)quinoline 5-HT(1) receptor ligands have been studied by elaboration of the series of dual 5-HT(1)-SSRIs reported previously. These new compounds display a different in vitro pharmacological profile with potent affinity across the 5-HT(1A), 5-HT(1B) and 5-HT(1D) receptors and selectivity against the serotonin transporter. Furthermore, they have improved pharmacokinetic profiles and CNS penetration.

Published

2008

39. WITHDRAWN: Bicyclic heteroarylpiperazines as selective brain penetrant 5-HT6 receptor antagonists

Author

Neil Upton, Vicky Holland, Andrew D. Medhurst, Geoffrey Stemp, Michael A. Briggs, Ashley Garner, Kim Winborn, Mervyn Thompson, Tania Buck, Steven Mark Bromidge, Dieter Hamprecht, Mahmood Ahmed, Stephen Moss, Lorraine Campbell, Nigel Deeks, Tania O. Stean, David R. Witty, Jenifer Powles, Christopher N. Johnson, Brenda K. Trail, Darren Jason Mitchell, Laurie J. Gordon, and Jon T. Seal

Subjects

chemistry.chemical_compound, Bicyclic molecule, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Drug Discovery, 5-HT6 receptor, Pharmaceutical Science, Molecular Medicine, Penetrant (biochemical), Molecular Biology, Biochemistry

Published

2005

40. Discovery of Potent, Orally Bioavailable, Selective 5-HT1A/B/DReceptor Antagonists.

Author

Simon E. Ward, Peter J. Eddershaw, Claire M. Scott, Laurie J. Gordon, Peter J. Lovell, Susan H. Moore, Paul W. Smith, Kathryn R. Starr, Kevin M. Thewlis, and Jeannette M. Watson

Published

2008