Your search keyword '"Pike, Kurt G."' showing total 18 results

1. The Identification of Potent, Selective, and Orally Available Inhibitors of Ataxia Telangiectasia Mutated (ATM) Kinase: The Discovery of AZD0156 (8-{6-[3-(Dimethylamino)propoxy]pyridin-3-yl}-3-methyl-1-(tetrahydro-2H-pyran-4-yl)-1,3-dihydro-2H-imidazo[4,5-c]quinolin-2-one)

Author

Pike, Kurt G., Barlaam, Bernard, Cadogan, Elaine, Campbell, Andrew, Yingxue Chen, Colclough, Nicola, Davies, Nichola L., de-Almeida, Camila, Degorce, Sebastien L., Didelot, Myriam, Dishington, Allan, Ducray, Richard, Durant, Stephen T., Hassall, Lorraine A., Holmes, Jane, Hughes, Gareth D., MacFaul, Philip A., Mulholland, Keith R., McGuire, Thomas M., and Ouvry, Gilles

Subjects

*ATAXIA telangiectasia, *KINASES, *XENOGRAFTS, *PHARMACOKINETICS, *QUINOLINE

Abstract

ATM inhibitors, such as 7, have demonstrated the antitumor potential of ATM inhibition when combined with DNA double-strand break-inducing agents in mouse xenograft models. However, the properties of 7 result in a relatively high predicted clinically efficacious dose. In an attempt to minimize attrition during clinical development, we sought to identify ATM inhibitors with a low predicted clinical dose (<50 mg) and focused on strategies to increase both ATM potency and predicted human pharmacokinetic half-life (predominantly through the increase of volume of distribution). These efforts resulted in the discovery of 64 (AZD0156), an exceptionally potent and selective inhibitor of ATM based on an imidazo[4,5-c]quinolin-2-one core. 64 has good preclinical phamacokinetics, a low predicted clinical dose, and a high maximum absorbable dose. 64 has been shown to potentiate the efficacy of the approved drugs irinotecan and olaparib in disease relevant mouse models and is currently undergoing clinical evaluation with these agents. [ABSTRACT FROM AUTHOR]

Published

2018

2. Discovery of AZD3147: A Potent, Selective Dual Inhibitor of mTORC1 and mTORC2.

Author

Pike, Kurt G., Morris, Jeff, Ruston, Linette, Pass, Sarah L., Greenwood, Ryan, Williams, Emma J., Demeritt, Julie, Culshaw, Janet D., Gill, Kristy, Pass, Martin, Finlay, M. Raymond V., Good, Catherine J., Roberts, Craig A., Currie, Gordon S., Blades, Kevin, Eden, Jonathan M., and Pearson, Stuart E.

Subjects

*MTOR protein, *DRUG development, *DRUG use testing, *MORPHOLINE, *LIVER cells, *MOLECULAR interactions

Abstract

High throughput screening followed by a lead generation campaign uncovered a novel series of urea containing morpholinopyrimidine compounds which act as potent and selective dual inhibitors of mTORC1 and mTORC2. We describe the continued compound optimization campaign for this series, in particular focused on identifying compounds with improved cellular potency, improved aqueous solubility, and good stability in human hepatocyte incubations. Knowledge from empirical SAR investigations was combined with an understanding of the molecular interactions in the crystal lattice to improve both cellular potency and solubility, and the composite parameters of LLE and pIC50-pSolubility were used to assess compound quality and progress. Predictive models were employed to efficiently mine the attractive chemical space identified resulting in the discovery of 42 (AZD3147), an extremely potent and selective dual inhibitor of mTORC1 and mTORC2 with physicochemical and pharmacokinetic properties suitable for development as a potential clinical candidate. [ABSTRACT FROM AUTHOR]

Published

2015

3. Optimization of potent and selective dual mTORC1 and mTORC2 inhibitors: The discovery of AZD8055 and AZD2014

Author

Pike, Kurt G., Malagu, Karine, Hummersone, Marc G., Menear, Keith A., Duggan, Heather M.E., Gomez, Sylvie, Martin, Niall M.B., Ruston, Linette, Pass, Sarah L., and Pass, Martin

Subjects

*RAPAMYCIN, *SOLUBILITY, *LIVER cells, *LIVER physiology, *METABOLISM, *AQUEOUS solutions

Abstract

Abstract: The optimization of a potent and highly selective series of dual mTORC1 and mTORC2 inhibitors is described. An initial focus on improving cellular potency whilst maintaining or improving other key parameters, such as aqueous solubility and margins over hERG IC50, led to the discovery of the clinical candidate AZD8055 (14). Further optimization, particularly aimed at reducing the rate of metabolism in human hepatocyte incubations, resulted in the discovery of the clinical candidate AZD2014 (21). [Copyright &y& Elsevier]

Published

2013

4. Design of a potent, soluble glucokinase activator with increased pharmacokinetic half-life

Author

Pike, Kurt G., Allen, Joanne V., Caulkett, Peter W.R., Clarke, David S., Donald, Craig S., Fenwick, Mark L., Johnson, Keith M., Johnstone, Craig, McKerrecher, Darren, Rayner, John W., Walker, Rolf P., and Wilson, Ingrid

Subjects

*DRUG design, *GLUCOKINASE, *PHARMACOKINETICS, *MOLECULAR structure, *SCAFFOLD proteins, *BIOAVAILABILITY, *TYPE 2 diabetes, *ORGANIC compounds

Abstract

Abstract: The continued optimization of a series of glucokinase activators is described, including attempts to understand the interplay between molecular structure and the composite parameter of unbound clearance. These studies resulted in the discovery of a new scaffold for glucokinase activators and further exploration of this scaffold led to the identification of GKA60. GKA60 maintains an excellent balance of potency and physical properties whilst possessing a significantly different, but complimentary, pre-clinical pharmacokinetic profile compared with the previously disclosed compound GKA50. [Copyright &y& Elsevier]

Published

2011

5. Synthesis of Highly Substituted Symmetrical 1,3-Dienes via Organocuprate Oxidation.

Author

Aves, Sarah J., O'Connell, Kieron M. G., Pike, Kurt G., and Spring, David R.

Subjects

*DIOLEFINS, *CHEMICAL synthesis, *GRIGNARD reagents, *OXIDATION kinetics, *HALIDES, *ALKENYL group, *COUPLING reactions (Chemistry) kinetics

Abstract

Oxidation of alkenyl organocuprates formed from alkenyl halides allows the formation of highly substituted symmetrical 1,3-dienes. Cuprates formed from organolithiums and Grignard reagents can be tolerated and the reaction proceeds with retention of alkenyl geometry. [ABSTRACT FROM AUTHOR]

Published

2012

6. The brain-penetrant clinical ATM inhibitor AZD1390 radiosensitizes and improves survival of preclinical brain tumor models.

Author

Durant, Stephen T., Li Zheng, Yingchun Wang, Kan Chen, Lingli Zhang, Tianwei Zhang, Zhenfan Yang, Riches, Lucy, Trinidad, Antonio G., Fok, Jacqueline H. L., Hunt, Tom, Pike, Kurt G., Wilson, Joanne, Smith, Aaron, Colclough, Nicola, Reddy, Venkatesh Pilla, Sykes, Andrew, Janefeldt, Annika, Johnström, Peter, and Varnäs, Katarina

Subjects

*KINASES, *GLIOMAS, *ANTINEOPLASTIC agents, *CELL cycle, *PHARMACOLOGY

Abstract

The article presents a study on the primary pharmacology of the clinical-grade ATM inhibitor AZD1390. It found that ATM-dependent DDR pathway activity is blocked by AZD1390 and induces G2 cell cycle phase accumulation, micronuclei, and apoptosis through combining with radiation. It radiosensitizes p53 mutant glioma cells with glioma and lung cancer cell lines.

Published

2018

7. Discovery of Novel 3-Quinoline Carboxamides as Potent, Selective, and Orally Bioavailable Inhibitors of Ataxia Telangiectasia Mutated (ATM) Kinase.

Author

Degorce, Sébastien L., Barlaam, Bernard, Cadogan, Elaine, Dishington, Allan, Ducray, Richard, Glossop, Steven C., Hassall, Lorraine A., Lach, Franck, Lau, Alan, McGuire, Thomas M., Nowak, Thorsten, Ouvry, Gilles, Pike, Kurt G., and Thomason, Andrew G.

Subjects

*QUINOLINE, *CARBOXAMIDES, *ATAXIA telangiectasia, *DRUG efficacy, *IRINOTECAN, *THERAPEUTICS

Abstract

A novel series of 3-quinoline carboxamides has been discovered and optimized as selective inhibitors of the ataxia telangiectasia mutated (ATM) kinase. From a modestly potent HTS hit (4), we identified molecules such as 6-[6-(methoxymethyl)-3-pyridinyl]-4-{[(1R)-1-(tetrahydro-2H-pyran-4-yl)ethyl]amino}-3-quinolinecarboxamide (72) and 7-fluoro-6-[6-(methoxymethyl)pyridin-3-yl]-4-{[(1S)-1-(1-methyl-1H-pyrazol-3-yl)ethyl]amino}quinoline-3-carboxamide (74) as potent and highly selective ATM inhibitors with overall ADME properties suitable for oral administration. 72 and 74 constitute excellent oral tools to probe ATM inhibition in vivo. Efficacy in combination with the DSB-inducing agent irinotecan was observed in a disease relevant model. [ABSTRACT FROM AUTHOR]

Published

2016

8. Synthesis of Novel Hydroxymethyl-Substituted Fused Heterocycles.

Author

Holmes, Jane L., Almeida, Lynsie, Barlaam, Bernard, Croft, Rosemary A., Dishington, Allan P., Gingipalli, Laksmaiah, Hassall, Lorraine A., Hawkins, Janet L., Ioannidis, Stephanos, Johannes, Jeffrey W., McGuire, Thomas M., Moore, Jane E., Patel, Anil, Pike, Kurt G., Pontz, Timothy, Xiaoyun Wu, Tao Wang, Hai-Jun Zhang, and Xiaolan Zheng

Subjects

*CHEMICAL synthesis, *HYDROXYMETHYL compounds, *HETEROCYCLIC compounds, *ISOQUINOLINE, *PQQ (Biochemistry)

Abstract

Examples of hydroxymethylated analogues of heteroaryl cores such as quinazolin-4-ones, isoquinolin-1(2H)-ones, pyrido[3,4- d]pyrimidin-4(3H)-ones, chromen-4-ones and pyrrolo[2,1-f][1,2,4]triazin- 4(3H)-ones are sparse or non-existent in the scientific literature. We have demonstrated that such compounds are accessible by using standard procedures from readily available raw materials. [ABSTRACT FROM AUTHOR]

Published

2016

9. Expedient synthesis of biologically important sulfonylmethyl pyrimidines.

Author

Blades, Kevin, Demeritt, Julie, Fillery, Shaun, Foote, Kevin M., Greenwood, Ryan, Gregson, Clare, Hassall, Lorraine A., McGuire, Thomas M., Pike, Kurt G., and Williams, Emma

Subjects

*PYRIMIDINE synthesis, *SULFONES, *MOIETIES (Chemistry), *DRUG development, *CHEMICALS, *CHEMICAL synthesis

Abstract

Abstract: Two novel synthetic strategies that allow rapid diversification of the sulfone moiety in sulfonylmethyl pyrimidines, a class of compounds with a wide range of biological activity, which are of interest in a wide variety of drug discovery programmes, are described. [Copyright &y& Elsevier]

Published

2014

10. Synthesis of 3-Substituted 2-Aminopyridines via Displacement of 3-Fluoro-2- nitropyridine.

Author

Culshaw, Janet D., Eden, Jonathan M., Ford, Susannah J., Hayter, Barry, Perkins, David R., and Pike, Kurt G.

Subjects

*HETEROCYCLIC chemistry, *HETEROCYCLIC compounds, *AMINOPYRIDINES, *REGIOSELECTIVITY (Chemistry), *CHEMICAL reactions, *ALIPHATIC amines

Abstract

An efficient method for the substitution of 3-fluoro-2-nitropyridine with a range of nitrogen-containing heterocycles and aliphatic amines is described. The reaction proceeds in a regioselective manner at moderate temperature and in reasonable yield. [ABSTRACT FROM AUTHOR]

Published

2012

11. Sulfonyl-morpholino-pyrimidines: SAR and development of a novel class of selective mTOR kinase inhibitor

Author

Finlay, M. Raymond V., Buttar, David, Critchlow, Susan E., Dishington, Allan P., Fillery, Shaun M., Fisher, Eric, Glossop, Steve C., Graham, Mark A., Johnson, Trevor, Lamont, Gillian M., Mutton, Simon, Perkins, Paula, Pike, Kurt G., and Slater., Anthony M.

Subjects

*PYRIMIDINES, *STRUCTURE-activity relationship in pharmacology, *DRUG development, *MTOR protein, *PROTEIN kinases, *HIGH throughput screening (Drug development), *HYDROGEN bonding

Abstract

Abstract: High throughput screening to identify inhibitors of the mTOR kinase revealed sulfonyl-morpholino-pyrimidine 1 as an attractive start point. The compound displayed good physicochemical properties and selectivity over related kinases such as PI3Kα. Library preparation of related analogs allowed the establishment of additional SAR understanding and in particular the requirement for a key hydrogen bond donor motif at the 4-position of the phenyl ring in compounds such as indole 19. Isosteric replacement of the indole functionality led to the identification of urea compounds such as 32 that show good levels of mTOR inhibition in both enzyme and cellular assays. [Copyright &y& Elsevier]

Published

2012

12. The discovery of N-cyclopropyl-4-methyl-3-[6-(4-methylpiperazin-1-yl)-4-oxoquinazolin-3(4H)-yl]benzamide (AZD6703), a clinical p38α MAP kinase inhibitor for the treatment of inflammatory diseases

Author

Brown, Dearg S., Cumming, John G., Bethel, Paul, Finlayson, Jonathan, Gerhardt, Stefan, Nash, Ian, Pauptit, Richard A., Pike, Kurt G., Reid, Alan, Snelson, Wendy, Swallow, Steve, and Thompson, Caroline

Subjects

*DRUG development, *CYCLOPROPYL compounds, *PIPERAZINE, *MITOGEN-activated protein kinases, *BENZAMIDE, *INFLAMMATION treatment

Abstract

Abstract: A novel, potent and selective quinazolinone series of inhibitors of p38α MAP kinase has been identified. Modifications designed to address the issues of poor aqueous solubility and high plasma protein binding as well as embedded aniline functionalities resulted in the identification of a clinical candidate N-cyclopropyl-4-methyl-3-[6-(4-methylpiperazin-1-yl)-4-oxoquinazolin-3(4H)-yl]benzamide (AZD6703). Optimisation was guided by understanding of the binding modes from X-ray crystallographic studies which showed a switch from DFG ‘out’ to DFG ‘in’ as the inhibitor size was reduced to improve overall properties. [Copyright &y& Elsevier]

Published

2012

13. Identification and optimisation of novel and selective small molecular weight kinase inhibitors of mTOR

Author

Menear, Keith A., Gomez, Sylvie, Malagu, Karine, Bailey, Christine, Blackburn, Kristel, Cockcroft, Xiao-Ling, Ewen, Sally, Fundo, Alexandra, Gall, Armelle Le, Hermann, Gesine, Sebastian, Luisa, Sunose, Mihiro, Presnot, Thomas, Torode, Eleanor, Hickson, Ian, Martin, Niall M.B., Smith, Graeme C.M., and Pike, Kurt G.

Subjects

*MOLECULAR weights, *TARGETED drug delivery, *PROTEIN kinases, *RAPAMYCIN, *TRIAZINES, *DRUG development, *ENZYME inhibitors

Abstract

Abstract: A pharmacophore mapping approach, derived from previous experience of PIKK family enzymes, was used to identify a hit series of selective inhibitors of the mammalian target of rapamycin (mTOR). Subsequent refinement of the SAR around this hit series based on a tri-substituted triazine scaffold has led to the discovery of potent and selective inhibitors of mTOR. [Copyright &y& Elsevier]

Published

2009

14. Identification and optimization of a novel series of selective PIP5K inhibitors.

Author

Andrews, David M., Cartic, Sharon, Cosulich, Sabina, Divecha, Nullin, Faulder, Paul, Flemington, Vikki, Kern, Oliver, Kettle, Jason G., MacDonald, Ellen, McKelvie, Jennifer, Pike, Kurt G., Roberts, Bryan, Rowlinson, Rachel, Smith, James M., Stockley, Martin, Swarbrick, Martin E., Treinies, Iris, and Waring, Michael J.

Subjects

*HIGH throughput screening (Drug development), *HUMAN biology

Abstract

[Display omitted] Phosphatidyl inositol (4,5)-bisphosphate (PI(4,5) P 2) plays several key roles in human biology and the lipid kinase that produces PI(4,5) P 2 , PIP5K, has been hypothesized to provide a potential therapeutic target of interest in the treatment of cancers. To better understand and explore the role of PIP5K in human cancers there remains an urgent need for potent and specific PIP5K inhibitor molecules. Following a high throughput screen of the AstraZeneca collection, a novel, moderately potent and selective inhibitor of PIP5K, 1 , was discovered. Detailed exploration of the SAR for this novel scaffold resulted in the considerable optimization of both potency for PIP5K, and selectivity over the closely related kinase PI3Kα, as well as identifying several opportunities for the continued optimization of drug-like properties. As a result, several high quality in vitro tool compounds were identified (8 , 20 and 25) that demonstrate the desired biochemical and cellular profiles required to aid better understanding of this complex area of biology. [ABSTRACT FROM AUTHOR]

Published

2022

15. Design of a potent, soluble glucokinase activator with excellent in vivo efficacy

Author

McKerrecher, Darren, Allen, Joanne V., Caulkett, Peter W.R., Donald, Craig S., Fenwick, Mark L., Grange, Emma, Johnson, Keith M., Johnstone, Craig, Jones, Clifford D., Pike, Kurt G., Rayner, John W., and Walker, Rolf P.

Subjects

*GLUCOKINASE, *BLOOD proteins, *PHARMACOKINETICS, *PROTEIN binding

Abstract

Abstract: The optimisation of a series of glucokinase activators is described, including attempts to uncouple the relationship between potency and plasma protein binding, and to better understand the key pharmacokinetic properties of the series. The use of unbound clearance as an optimisation parameter facilitated the identification of GKA50, a compound which combines excellent potency and pharmacokinetics with good free drug levels and solubility, and exhibits in vivo efficacy at 1mg/kg po in an acute rat OGTT model. [Copyright &y& Elsevier]

Published

2006

16. A novel series of p38 MAP kinase inhibitors for the potential treatment of rheumatoid arthritis

Author

Brown, Dearg S., Belfield, Andrew J., Brown, George R., Campbell, Douglas, Foubister, Alan, Masters, David J., Pike, Kurt G., Snelson, Wendy L., and Wells, Stuart L.

Published

2004

17. Free energy perturbation in the design of EED ligands as inhibitors of polycomb repressive complex 2 (PRC2) methyltransferase.

Author

O' Donovan, Daniel H., Gregson, Clare, Packer, Martin J., Greenwood, Ryan, Pike, Kurt G., Kawatkar, Sameer, Bloecher, Andrew, Robinson, James, Read, Jon, Code, Erin, Hsu, Jessie Hao-Ru, Shen, Minhui, Woods, Haley, Barton, Peter, Fillery, Shaun, Williamson, Beth, Rawlins, Philip B., and Bagal, Sharan K.

Subjects

*LIGANDS (Biochemistry), *SURFACE plasmon resonance, *BINDING sites

Abstract

[Display omitted] • A series of triazolopyrimidine EED ligands is reported which explores a novel pocket within the binding site. • Free Energy Perturbation (FEP) calculations were used to predict their affinity, as verified by surface plasmon resonance (SPR) • A synthetic approach incorporating late-stage functionalization (LSF) enabled rapid exploration of SAR. • New ligands retain high affinity for EED while improving their physicochemical properties. Free Energy Perturbation (FEP) calculations can provide high-confidence predictions of the interaction strength between a ligand and its protein target. We sought to explore a series of triazolopyrimidines which bind to the EED subunit of the PRC2 complex as potential anticancer therapeutics, using FEP calculations to inform compound design. Combining FEP predictions with a late-stage functionalisation (LSF) inspired synthetic approach allowed us to rapidly evaluate structural modifications in a previously unexplored region of the EED binding site. This approach generated a series of novel triazolopyrimidine EED ligands with improved physicochemical properties and which inhibit PRC2 methyltransferase activity in a cancer-relevant G401 cell line. [ABSTRACT FROM AUTHOR]

Published

2021

18. ChemInform Abstract: Synthesis of 3-Substituted 2-Aminopyridines via Displacement of 3-Fluoro-2-nitropyridine.

Author

Culshaw, Janet D., Eden, Jonathan M., Ford, Susannah J., Hayter, Barry, Perkins, David R., and Pike, Kurt G.

Abstract

The fluorine in title compound (I) can be substituted by aliphatic amines or various nitrogen-containing heterocycles. [ABSTRACT FROM AUTHOR]

Published

2012