Your search keyword '"David M. Andrews"' showing total 6 results

1. Discovery of potent, selective small molecule inhibitors of α-subtype of type III phosphatidylinositol-4-kinase (PI4KIIIα)

Author

David M. Andrews, Graeme R. Robb, Martin E. Swarbrick, Jennifer C. McKelvie, James M. Smith, Michael J. Waring, and Piotr Raubo

Subjects

Models, Molecular, Stereochemistry, Inositol Phosphates, Clinical Biochemistry, Pharmaceutical Science, Stimulation, Biochemistry, Biological pathway, Minor Histocompatibility Antigens, Small Molecule Libraries, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Potency, Humans, Phosphatidylinositol, Enzyme Inhibitors, Molecular Biology, Platelet-Derived Growth Factor, biology, Kinase, Organic Chemistry, Small molecule, In vitro, High-Throughput Screening Assays, Phosphotransferases (Alcohol Group Acceptor), chemistry, Drug Design, biology.protein, Molecular Medicine, Platelet-derived growth factor receptor, Signal Transduction

Abstract

The discovery and optimisation of novel, potent and selective small molecule inhibitors of the α-isoform of type III phosphatidylinositol-4-kinase (PI4Kα) are described. Lead compounds show cellular activity consistent with their PI4Kα potency inhibiting the accumulation of IP1 after PDGF stimulation and reducing cellular PIP, PIP2 and PIP3 levels. Hence, these compounds are useful in vitro tools to delineate the complex biological pathways involved in signalling through PI4Kα.

Published

2015

2. The discovery of AZD5597, a potent imidazole pyrimidine amide CDK inhibitor suitable for intravenous dosing

Author

Kin Yip Tam, David Alan Rudge, Julie A. Tucker, Louise Moss, Barker Andrew John, Clifford David Jones, Peter B. Simpson, Alexandra McGregor, David M. Andrews, Michael A. Walker, Kevin Blades, Catherine Geh, Swain Michael Lingard, S J East, Keith M. Johnson, Heather M. McFarland, Mark A. Graham, Sarah A. Loddick, and Paula Daunt

Subjects

ERG1 Potassium Channel, Pyrimidine, Clinical Biochemistry, hERG, Molecular Conformation, Pharmaceutical Science, Crystallography, X-Ray, Biochemistry, chemistry.chemical_compound, Cyclin-dependent kinase, Cell Line, Tumor, Drug Discovery, Imidazole, Humans, Protein Isoforms, Infusions, Intravenous, Molecular Biology, Protein Kinase Inhibitors, Cyclin-Dependent Kinase Inhibitor Proteins, biology, Chemistry, Chemistry, Physical, Organic Chemistry, Imidazoles, Biological activity, Amides, Ether-A-Go-Go Potassium Channels, Pyrimidines, Models, Chemical, Enzyme inhibitor, Drug Design, Lipophilicity, biology.protein, Molecular Medicine, CDK inhibitor, Neoplasm Transplantation

Abstract

The development of a novel series of imidazole pyrimidine amides as cyclin-dependent kinase (CDK) inhibitors is described. Optimisation of inhibitory potency against multiple CDK's (1, 2 and 9) resulted in imidazole pyrimidine amides with potent in vitro anti-proliferative effects against a range of cancer cell lines. Excellent physiochemical properties and large margins against inhibition of CYP isoforms and the hERG ion channel were achieved by modification of lipophilicity and amine basicity. A candidate with disease model activity in human cancer cell line xenografts and with suitable physiochemical and pharmacokinetic profiles for intravenous (i.v.) dosing was selected for further development as AZD5597.

Published

2008

3. Imidazole pyrimidine amides as potent, orally bioavailable cyclin-dependent kinase inhibitors

Author

Kate Byth, Barker Andrew John, David M. Andrews, Marie Willaing Johannsen, M. Raymond V. Finlay, Clive Green, Hazel M. Weir, Catherine Geh, Kevin Blades, Clifford David Jones, and Michael A. Walker

Subjects

Male, Pyrimidine, medicine.drug_class, Clinical Biochemistry, hERG, Pharmaceutical Science, Administration, Oral, Mice, Nude, Carboxamide, Biochemistry, chemistry.chemical_compound, Inhibitory Concentration 50, Mice, In vivo, Cyclin-dependent kinase, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Rats, Wistar, Molecular Biology, Cyclin-Dependent Kinase Inhibitor Proteins, biology, Organic Chemistry, Cyclin-dependent kinase 2, Imidazoles, Rats, Pyrimidines, chemistry, Enzyme inhibitor, Lipophilicity, biology.protein, Molecular Medicine, Female, Drug Screening Assays, Antitumor

Abstract

The development of a novel series of imidazole pyrimidine amides as cyclin-dependent kinase (CDK) inhibitors is described. The series was found to have much improved CDK2 inhibition and potent in vitro anti-proliferative effects against cancer cell lines. Control of overall lipophilicity was important to achieve good in vitro potency along with acceptable physiochemical properties and margins against inhibition of both CYP isoforms and the hERG potassium ion channel. A compound with an attractive overall balance of properties was profiled in vivo and possessed suitable physiochemical and pharmacokinetic profiles for oral dosing.

Published

2008

4. Imidazoles: SAR and development of a potent class of cyclin-dependent kinase inhibitors

Author

Janet D. Culshaw, Jason Breed, M. Raymond V. Finlay, Julie A. Tucker, J.J. Stanway, Claire Brassington, Kate Byth, Andy Barker, Malcolm Anderson, Nash Ian Alun, Richard A. Pauptit, Andrew D. Roberts, Andrew Peter Thomas, Hazel M. Weir, Michael A. Walker, David M. Andrews, Nicholas John Newcombe, Eric Fisher, Dave W. Heaton, Helen H.J. McMiken, Clive Green, and Sandra E. Oakes

Subjects

Chemistry, Pharmaceutical, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Cell Cycle Proteins, Crystallography, X-Ray, Biochemistry, Sulfone, chemistry.chemical_compound, Inhibitory Concentration 50, Mice, Structure-Activity Relationship, Cyclin-dependent kinase, Drug Discovery, Transferase, Imidazole, Animals, Humans, Molecular Biology, chemistry.chemical_classification, Aniline Compounds, biology, Kinase, Organic Chemistry, Imidazoles, Hydrogen Bonding, Cyclin-Dependent Kinases, Enzyme, chemistry, Models, Chemical, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine, CDK inhibitor

Abstract

An imidazole series of cyclin-dependent kinase (CDK) inhibitors has been developed. Protein inhibitor structure determination has provided an understanding of the emerging structure activity trends for the imidazole series. The introduction of a methyl sulfone at the aniline terminus led to a more orally bioavailable CDK inhibitor that was progressed into clinical development.

Published

2008

5. Imidazole piperazines: SAR and development of a potent class of cyclin-dependent kinase inhibitors with a novel binding mode

Author

David William AstraZeneca R D Alderley Heaton, Hazel M. Weir, Julie A. Tucker, Eric Fisher, Galith Karoutchi, Sarah A. Loddick, Mark A. Graham, Michael Dennis, Clive Green, Barker Andrew John, David M. Andrews, Andrew D. Roberts, M. Raymond V. Finlay, Rémy Morgentin, and David G. Acton

Subjects

Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Mice, Nude, Antineoplastic Agents, Biochemistry, Chemical synthesis, Piperazines, Mice, Structure-Activity Relationship, Cyclin-dependent kinase, Drug Discovery, Structure–activity relationship, Transferase, Animals, Combinatorial Chemistry Techniques, Binding site, Enzyme Inhibitors, Molecular Biology, chemistry.chemical_classification, Aspartic Acid, Binding Sites, biology, Molecular Structure, Chemistry, Kinase, Organic Chemistry, Cyclin-dependent kinase 2, Cyclin-Dependent Kinase 2, Imidazoles, Xenograft Model Antitumor Assays, Cyclin-Dependent Kinases, Enzyme, Drug Design, biology.protein, Molecular Medicine, Drug Screening Assays, Antitumor

Abstract

A piperazine series of cyclin-dependent kinase (CDK) inhibitors have been identified. The compounds exhibit excellent physiochemical properties and a novel binding mode, whereby a bridging interaction via a water molecule with Asp 86 of CDK2, leads to selectivity for the CDK family of enzymes over other kinases. Piperazines 2e and 2i were subsequently shown to inhibit tumour growth when dosed orally in a nude mouse xenograft study. Additional chemical series that exploit this unexpected interaction with Asp 86 are also described.

Published

2008

6. Design and campaign synthesis of piperidine- and thiazole-based histone deacetylase inhibitors

Author

Christine M. Chresta, Greg Carr, Michael J. Waring, S J East, Zbigniew Stanley Matusiak, David M. Andrews, Stokes Elaine Sophie Elizabeth, Craig A. Roberts, and Madeleine C. Brady

Subjects

Models, Molecular, medicine.drug_class, Clinical Biochemistry, Pharmaceutical Science, Antineoplastic Agents, Pharmacology, Crystallography, X-Ray, Biochemistry, Histone Deacetylases, chemistry.chemical_compound, Mice, Structure-Activity Relationship, Dogs, Piperidines, Cell Line, Tumor, Drug Discovery, medicine, Potency, Structure–activity relationship, Animals, Humans, Enzyme Inhibitors, Benzamide, Thiazole, Molecular Biology, biology, Dose-Response Relationship, Drug, Molecular Structure, Organic Chemistry, Histone deacetylase inhibitor, Xenograft Model Antitumor Assays, Rats, Histone Deacetylase Inhibitors, Thiazoles, Histone, chemistry, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine, Histone deacetylase

Abstract

A lead benzamide, 3, was identified as a potent and low molecular weight histone deacetylase (HDAC) inhibitor. Optimization led to 16d, demonstrating an excellent balance of efficacy and non-efficacy properties, along with very desirable in vivo DMPK. The final compounds presented are >1000-fold more potent than the initial screen hit, an improvement in potency which was achieved with a concomitant significant improvement in all the main non-efficacy properties.

Published

2008