Your search keyword '"Kwai-Ming J. Cheung"' showing total 41 results

1. Discovering cell-active BCL6 inhibitors: effectively combining biochemical HTS with multiple biophysical techniques, X-ray crystallography and cell-based assays

Author

Olivier A. Pierrat, Manjuan Liu, Gavin W. Collie, Kartika Shetty, Matthew J. Rodrigues, Yann-Vaï Le Bihan, Emma A. Gunnell, P. Craig McAndrew, Mark Stubbs, Martin G. Rowlands, Norhakim Yahya, Erald Shehu, Rachel Talbot, Lisa Pickard, Benjamin R. Bellenie, Kwai-Ming J. Cheung, Ludovic Drouin, Paolo Innocenti, Hannah Woodward, Owen A. Davis, Matthew G. Lloyd, Ana Varela, Rosemary Huckvale, Fabio Broccatelli, Michael Carter, David Galiwango, Angela Hayes, Florence I. Raynaud, Christopher Bryant, Steven Whittaker, Olivia W. Rossanese, Swen Hoelder, Rosemary Burke, and Rob L. M. van Montfort

Subjects

Medicine, Science

Abstract

Abstract By suppressing gene transcription through the recruitment of corepressor proteins, B-cell lymphoma 6 (BCL6) protein controls a transcriptional network required for the formation and maintenance of B-cell germinal centres. As BCL6 deregulation is implicated in the development of Diffuse Large B-Cell Lymphoma, we sought to discover novel small molecule inhibitors that disrupt the BCL6-corepressor protein–protein interaction (PPI). Here we report our hit finding and compound optimisation strategies, which provide insight into the multi-faceted orthogonal approaches that are needed to tackle this challenging PPI with small molecule inhibitors. Using a 1536-well plate fluorescence polarisation high throughput screen we identified multiple hit series, which were followed up by hit confirmation using a thermal shift assay, surface plasmon resonance and ligand-observed NMR. We determined X-ray structures of BCL6 bound to compounds from nine different series, enabling a structure-based drug design approach to improve their weak biochemical potency. We developed a time-resolved fluorescence energy transfer biochemical assay and a nano bioluminescence resonance energy transfer cellular assay to monitor cellular activity during compound optimisation. This workflow led to the discovery of novel inhibitors with respective biochemical and cellular potencies (IC50s) in the sub-micromolar and low micromolar range.

Published

2022

2. Discovery of an In Vivo Chemical Probe for BCL6 Inhibition by Optimization of Tricyclic Quinolinones

Author

Alice C. Harnden, Owen A. Davis, Gary M. Box, Angela Hayes, Louise D. Johnson, Alan T. Henley, Alexis K. de Haven Brandon, Melanie Valenti, Kwai-Ming J. Cheung, Alfie Brennan, Rosemary Huckvale, Olivier A. Pierrat, Rachel Talbot, Michael D. Bright, Hafize Aysin Akpinar, Daniel S. J. Miller, Dalia Tarantino, Sharon Gowan, Selby de Klerk, Peter Craig McAndrew, Yann-Vaï Le Bihan, Mirco Meniconi, Rosemary Burke, Vladimir Kirkin, Rob L. M. van Montfort, Florence I. Raynaud, Olivia W. Rossanese, Benjamin R. Bellenie, and Swen Hoelder

Subjects

Drug Discovery, Molecular Medicine

Published

2023

3. Optimizing Shape Complementarity Enables the Discovery of Potent Tricyclic BCL6 Inhibitors

Author

Owen A. Davis, Kwai-Ming J. Cheung, Alfie Brennan, Matthew G. Lloyd, Matthew J. Rodrigues, Olivier A. Pierrat, Gavin W. Collie, Yann-Vaï Le Bihan, Rosemary Huckvale, Alice C. Harnden, Ana Varela, Michael D. Bright, Paul Eve, Angela Hayes, Alan T. Henley, Michael D. Carter, P. Craig McAndrew, Rachel Talbot, Rosemary Burke, Rob L. M. van Montfort, Florence I. Raynaud, Olivia W. Rossanese, Mirco Meniconi, Benjamin R. Bellenie, and Swen Hoelder

Subjects

BTB-POZ Domain, Drug Discovery, Proto-Oncogene Proteins c-bcl-6, Molecular Medicine, Protein Binding

Abstract

To identify new chemical series with enhanced binding affinity to the BTB domain of B-cell lymphoma 6 protein, we targeted a subpocket adjacent to Val18. With no opportunities for strong polar interactions, we focused on attaining close shape complementarity by ring fusion onto our quinolinone lead series. Following exploration of different sized rings, we identified a conformationally restricted core which optimally filled the available space, leading to potent BCL6 inhibitors. Through X-ray structure-guided design, combined with efficient synthetic chemistry to make the resulting novel core structures, a300-fold improvement in activity was obtained by the addition of seven heavy atoms.

Published

2022

4. Improved Binding Affinity and Pharmacokinetics Enable Sustained Degradation of BCL6 In Vivo

Author

Rosemary Huckvale, Alice C. Harnden, Kwai-Ming J. Cheung, Olivier A. Pierrat, Rachel Talbot, Gary M. Box, Alan T. Henley, Alexis K. de Haven Brandon, Albert E. Hallsworth, Michael D. Bright, Hafize Aysin Akpinar, Daniel S. J. Miller, Dalia Tarantino, Sharon Gowan, Angela Hayes, Emma A. Gunnell, Alfie Brennan, Owen A. Davis, Louise D. Johnson, Selby de Klerk, Craig McAndrew, Yann-Vaï Le Bihan, Mirco Meniconi, Rosemary Burke, Vladimir Kirkin, Rob L. M. van Montfort, Florence I. Raynaud, Olivia W. Rossanese, Benjamin R. Bellenie, and Swen Hoelder

Subjects

Gene Expression Regulation, Neoplastic, Mice, Carcinogenesis, Drug Discovery, Proto-Oncogene Proteins c-bcl-6, Animals, Humans, Molecular Medicine

Abstract

The transcriptional repressor BCL6 is an oncogenic driver found to be deregulated in lymphoid malignancies. Herein, we report the optimization of our previously reported benzimidazolone molecular glue-type degrader

Published

2022

5. Adobe PDF - MCT-07-0149--Suppl_Data.pdf from Inhibition of the heat shock protein 90 molecular chaperone in vitro and in vivo by novel, synthetic, potent resorcinylic pyrazole/isoxazole amide analogues

Author

Paul Workman, Martin Drysdale, Sue Eccles, Florence Raynaud, Edward McDonald, Keith Jones, Laurence Pearl, Wynne Aherne, Roderick E. Hubbard, Nicolas Foloppe, Allan Surgenor, Lisa Wright, Julie E. Cansfield, Xavier Barril, Paul A. Brough, Brian Dymock, Anthea Hardcastle, Angela Hayes, Karen James, Andrew Kalusa, Kwai-Ming J. Cheung, Thomas P. Matthews, Gary Box, Joanna L. Holmes, Marissa V. Powers, Kathy Boxall, Chrisostomos Prodromou, and Swee Y. Sharp

Abstract

Adobe PDF - MCT-07-0149--Suppl_Data.pdf from Inhibition of the heat shock protein 90 molecular chaperone in vitro and in vivo by novel, synthetic, potent resorcinylic pyrazole/isoxazole amide analogues

Published

2023

6. Data from Inhibition of the heat shock protein 90 molecular chaperone in vitro and in vivo by novel, synthetic, potent resorcinylic pyrazole/isoxazole amide analogues

Author

Paul Workman, Martin Drysdale, Sue Eccles, Florence Raynaud, Edward McDonald, Keith Jones, Laurence Pearl, Wynne Aherne, Roderick E. Hubbard, Nicolas Foloppe, Allan Surgenor, Lisa Wright, Julie E. Cansfield, Xavier Barril, Paul A. Brough, Brian Dymock, Anthea Hardcastle, Angela Hayes, Karen James, Andrew Kalusa, Kwai-Ming J. Cheung, Thomas P. Matthews, Gary Box, Joanna L. Holmes, Marissa V. Powers, Kathy Boxall, Chrisostomos Prodromou, and Swee Y. Sharp

Abstract

Although the heat shock protein 90 (HSP90) inhibitor 17-allylamino-17-demethoxygeldanamycin (17-AAG) shows clinical promise, potential limitations encourage development of alternative chemotypes. We discovered the 3,4-diarylpyrazole resorcinol CCT018159 by high-throughput screening and used structure-based design to generate more potent pyrazole amide analogues, exemplified by VER-49009. Here, we describe the detailed biological properties of VER-49009 and the corresponding isoxazole VER-50589. X-ray crystallography showed a virtually identical HSP90 binding mode. However, the dissociation constant (Kd) of VER-50589 was 4.5 ± 2.2 nmol/L compared with 78.0 ± 10.4 nmol/L for VER-49009, attributable to higher enthalpy for VER-50589 binding. A competitive binding assay gave a lower IC50 of 21 ± 4 nmol/L for VER-50589 compared with 47 ± 9 nmol/L for VER-49009. Cellular uptake of VER-50589 was 4-fold greater than for VER-49009. Mean cellular antiproliferative GI50 values for VER-50589 and VER-49009 for a human cancer cell line panel were 78 ± 15 and 685 ± 119 nmol/L, respectively, showing a 9-fold potency gain for the isoxazole. Unlike 17-AAG, but as with CCT018159, cellular potency of these analogues was independent of NAD(P)H:quinone oxidoreductase 1/DT-diaphorase and P-glycoprotein expression. Consistent with HSP90 inhibition, VER-50589 and VER-49009 caused induction of HSP72 and HSP27 alongside depletion of client proteins, including C-RAF, B-RAF, and survivin, and the protein arginine methyltransferase PRMT5. Both caused cell cycle arrest and apoptosis. Extent and duration of pharmacodynamic changes in an orthotopic human ovarian carcinoma model confirmed the superiority of VER-50589 over VER-49009. VER-50589 accumulated in HCT116 human colon cancer xenografts at levels above the cellular GI50 for 24 h, resulting in 30% growth inhibition. The results indicate the therapeutic potential of the resorcinylic pyrazole/isoxazole amide analogues as HSP90 inhibitors. [Mol Cancer Ther 2007;6(4):1198–211]

Published

2023

7. Supplementary Fig 4 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Author

Spiros Linardopoulos, Rob L.M. Van Montfort, Julian Blagg, Swen Hoelder, Rosemary Burke, Paul Workman, Grace Mak, Kathy Boxall, Jessica Schmitt, Amy Wood, Craig McAndrew, Kwai-Ming J. Cheung, Sébastien Naud, Amir Faisal, Isaac M. Westwood, and Mark D. Gurden

Abstract

CCT251455-resistant HCT116 clones.

Published

2023

8. Supplementary Fig 6 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Author

Spiros Linardopoulos, Rob L.M. Van Montfort, Julian Blagg, Swen Hoelder, Rosemary Burke, Paul Workman, Grace Mak, Kathy Boxall, Jessica Schmitt, Amy Wood, Craig McAndrew, Kwai-Ming J. Cheung, Sébastien Naud, Amir Faisal, Isaac M. Westwood, and Mark D. Gurden

Abstract

ddPCR analysis of drug-resistance mutations shows they are pre-existing in cancer cell lines and quickly introduced into a population of HCT116 cells.

Published

2023

9. Supplementary Materials, Table 1 and Figures 1-3 from In vitro Biological Characterization of a Novel, Synthetic Diaryl Pyrazole Resorcinol Class of Heat Shock Protein 90 Inhibitors

Author

Paul Workman, Edward McDonald, Wynne Aherne, Sue Eccles, Laurence Pearl, Richard Marais, Florence Raynaud, Angela Hayes, Karen Ball, Kwai-Ming J. Cheung, Thomas P. Matthews, Lisa Patterson, Sharon Sanderson, Gary Box, Paul A. Clarke, Marissa Powers, Alison Maloney, S. Mark Roe, Chrisostomos Prodromou, Martin Rowlands, Kathy Boxall, and Swee Y. Sharp

Abstract

Supplementary Materials, Table 1 and Figures 1-3 from In vitro Biological Characterization of a Novel, Synthetic Diaryl Pyrazole Resorcinol Class of Heat Shock Protein 90 Inhibitors

Published

2023

10. Supplementary Tables S1-S10 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Author

Spiros Linardopoulos, Rob L.M. Van Montfort, Julian Blagg, Swen Hoelder, Rosemary Burke, Paul Workman, Grace Mak, Kathy Boxall, Jessica Schmitt, Amy Wood, Craig McAndrew, Kwai-Ming J. Cheung, Sébastien Naud, Amir Faisal, Isaac M. Westwood, and Mark D. Gurden

Abstract

Tables of biochemical and viability assays of resistant cell clones, fractional abundance of MPS1 mutants in different human cancer cell lines and refinement statistics of crystal structures of different MPS1 domains.

Published

2023

11. Supplementary Fig 2 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Author

Spiros Linardopoulos, Rob L.M. Van Montfort, Julian Blagg, Swen Hoelder, Rosemary Burke, Paul Workman, Grace Mak, Kathy Boxall, Jessica Schmitt, Amy Wood, Craig McAndrew, Kwai-Ming J. Cheung, Sébastien Naud, Amir Faisal, Isaac M. Westwood, and Mark D. Gurden

Abstract

Expression of the p.M600T, p.Y568C and p.C604W MPS1 mutant constructs in DLD1 Flp-In TRex cells recues the spindle assembly checkpoint defect following AZ3146 treatment.

Published

2023

12. Supplementary Fig 3 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Author

Spiros Linardopoulos, Rob L.M. Van Montfort, Julian Blagg, Swen Hoelder, Rosemary Burke, Paul Workman, Grace Mak, Kathy Boxall, Jessica Schmitt, Amy Wood, Craig McAndrew, Kwai-Ming J. Cheung, Sébastien Naud, Amir Faisal, Isaac M. Westwood, and Mark D. Gurden

Abstract

CCT251455 kills cancer cells by inhibiting the kinetochore recruitment of SAC protein.

Published

2023

13. Data from In vitro Biological Characterization of a Novel, Synthetic Diaryl Pyrazole Resorcinol Class of Heat Shock Protein 90 Inhibitors

Author

Paul Workman, Edward McDonald, Wynne Aherne, Sue Eccles, Laurence Pearl, Richard Marais, Florence Raynaud, Angela Hayes, Karen Ball, Kwai-Ming J. Cheung, Thomas P. Matthews, Lisa Patterson, Sharon Sanderson, Gary Box, Paul A. Clarke, Marissa Powers, Alison Maloney, S. Mark Roe, Chrisostomos Prodromou, Martin Rowlands, Kathy Boxall, and Swee Y. Sharp

Abstract

The molecular chaperone heat shock protein 90 (HSP90) has emerged as an exciting molecular target. Derivatives of the natural product geldanamycin, such as 17-allylamino-17-demethoxy-geldanamycin (17-AAG), were the first HSP90 ATPase inhibitors to enter clinical trial. Synthetic small-molecule HSP90 inhibitors have potential advantages. Here, we describe the biological properties of the lead compound of a new class of 3,4-diaryl pyrazole resorcinol HSP90 inhibitor (CCT018159), which we identified by high-throughput screening. CCT018159 inhibited human HSP90β with comparable potency to 17-AAG and with similar ATP-competitive kinetics. X-ray crystallographic structures of the NH2-terminal domain of yeast Hsp90 complexed with CCT018159 or its analogues showed binding properties similar to radicicol. The mean cellular GI50 value of CCT018159 across a panel of human cancer cell lines, including melanoma, was 5.3 μmol/L. Unlike 17-AAG, the in vitro antitumor activity of the pyrazole resorcinol analogues is independent of NQO1/DT-diaphorase and P-glycoprotein expression. The molecular signature of HSP90 inhibition, comprising increased expression of HSP72 protein and depletion of ERBB2, CDK4, C-RAF, and mutant B-RAF, was shown by Western blotting and quantified by time-resolved fluorescent-Cellisa in human cancer cell lines treated with CCT018159. CCT018159 caused cell cytostasis associated with a G1 arrest and induced apoptosis. CCT018159 also inhibited key endothelial and tumor cell functions implicated in invasion and angiogenesis. Overall, we have shown that diaryl pyrazole resorcinols exhibited similar cellular properties to 17-AAG with potential advantages (e.g., aqueous solubility, independence from NQO1 and P-glycoprotein). These compounds form the basis for further structure-based optimization to identify more potent inhibitors suitable for clinical development. [Cancer Res 2007;67(5):2206–16]

Published

2023

14. Supplementary experimental procedures figure legends and references from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Author

Spiros Linardopoulos, Rob L.M. Van Montfort, Julian Blagg, Swen Hoelder, Rosemary Burke, Paul Workman, Grace Mak, Kathy Boxall, Jessica Schmitt, Amy Wood, Craig McAndrew, Kwai-Ming J. Cheung, Sébastien Naud, Amir Faisal, Isaac M. Westwood, and Mark D. Gurden

Abstract

Description of the supplementary experimental procedures figure legends and references

Published

2023

15. Supplementary Fig 5 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Author

Spiros Linardopoulos, Rob L.M. Van Montfort, Julian Blagg, Swen Hoelder, Rosemary Burke, Paul Workman, Grace Mak, Kathy Boxall, Jessica Schmitt, Amy Wood, Craig McAndrew, Kwai-Ming J. Cheung, Sébastien Naud, Amir Faisal, Isaac M. Westwood, and Mark D. Gurden

Abstract

Crystal structures of AZD3146 and ONCOII bound to MPS1-KD.

Published

2023

16. Supplementary Fig 1 from Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Author

Spiros Linardopoulos, Rob L.M. Van Montfort, Julian Blagg, Swen Hoelder, Rosemary Burke, Paul Workman, Grace Mak, Kathy Boxall, Jessica Schmitt, Amy Wood, Craig McAndrew, Kwai-Ming J. Cheung, Sébastien Naud, Amir Faisal, Isaac M. Westwood, and Mark D. Gurden

Abstract

Expression of the p.S611G, p.I531M and Dbl MPS1 mutant constructs in DLD1 Flp-In TRex cells recues the spindle assembly checkpoint defect following AZ3146 treatment.

Published

2023

17. Into Deep Water: Optimizing BCL6 Inhibitors by Growing into a Solvated Pocket

Author

Rob L. M. van Montfort, Kwai-Ming J. Cheung, L. Johnson, Mirco Meniconi, Florence I. Raynaud, P. Craig McAndrew, Rosemary Huckvale, Gavin W. Collie, Alan T. Henley, Olivier A. Pierrat, Emma Gunnell, Michael Carter, Matthew J. Rodrigues, Yann-Vaï Le Bihan, Mahad Gatti Iou, Matthew Garth Lloyd, Angela Hayes, Benjamin R. Bellenie, Rosemary Burke, Rachel Talbot, Olivia W. Rossanese, Michael D. Bright, Swen Hoelder, and Owen Alexander Davis

Subjects

Hydrogen bond, Antineoplastic Agents, Hydrogen Bonding, Crystallography, X-Ray, Combinatorial chemistry, Article, Deep water, chemistry.chemical_compound, Structure-Activity Relationship, chemistry, Solubility, Drug Design, Drug Discovery, Proto-Oncogene Proteins c-bcl-6, Molecular Medicine, Molecule, Bound water, Humans, Lead compound

Abstract

We describe the optimization of modestly active starting points to potent inhibitors of BCL6 by growing into a subpocket, which was occupied by a network of five stably bound water molecules. Identifying potent inhibitors required not only forming new interactions in the subpocket but also perturbing the water network in a productive, potency-increasing fashion while controlling the physicochemical properties. We achieved this goal in a sequential manner by systematically probing the pocket and the water network, ultimately achieving a 100-fold improvement of activity. The most potent compounds displaced three of the five initial water molecules and formed hydrogen bonds with the remaining two. Compound 25 showed a promising profile for a lead compound with submicromolar inhibition of BCL6 in cells and satisfactory pharmacokinetic (PK) properties. Our work highlights the importance of finding productive ways to perturb existing water networks when growing into solvent-filled protein pockets.

Published

2021

18. Achieving In Vivo Target Depletion through the Discovery and Optimization of Benzimidazolone BCL6 Degraders

Author

Hannah Woodward, Kwai-Ming J. Cheung, Paolo Innocenti, L. Johnson, Benjamin R. Bellenie, Florence I. Raynaud, Olivia W. Rossanese, Sharon Gowan, Vladimir Kirkin, Michael D. Bright, Alan T. Henley, Gavin W. Collie, Selby de Klerk, Olivier A. Pierrat, Rachel Talbot, Michael Carter, Yann-Vaï Le Bihan, Angela Hayes, Matthew Garth Lloyd, Manjuan Liu, Swen Hoelder, Rosemary Burke, Erald Shehu, Ana Varela, Matthew J. Rodrigues, Owen Alexander Davis, P. Craig McAndrew, Kartika N. Shetty, Gary Box, and Rob L. M. van Montfort

Subjects

0303 health sciences, Chemistry, Germinal center, medicine.disease, medicine.disease_cause, BCL6, 01 natural sciences, 0104 chemical sciences, Lymphoma, 010404 medicinal & biomolecular chemistry, 03 medical and health sciences, Liver metabolism, immune system diseases, Cell culture, In vivo, hemic and lymphatic diseases, Drug Discovery, Transcriptional Repressor, medicine, Cancer research, Molecular Medicine, Carcinogenesis, 030304 developmental biology

Abstract

Deregulation of the transcriptional repressor BCL6 enables tumorigenesis of germinal center B-cells, and hence BCL6 has been proposed as a therapeutic target for the treatment of diffuse large B-cell lymphoma (DLBCL). Herein we report the discovery of a series of benzimidazolone inhibitors of the protein-protein interaction between BCL6 and its co-repressors. A subset of these inhibitors were found to cause rapid degradation of BCL6, and optimization of pharmacokinetic properties led to the discovery of 5-((5-chloro-2-((3R,5S)-4,4-difluoro-3,5-dimethylpiperidin-1-yl)pyrimidin-4-yl)amino)-3-(3-hydroxy-3-methylbutyl)-1-methyl-1,3-dihydro-2H-benzo[d]imidazol-2-one (CCT369260), which reduces BCL6 levels in a lymphoma xenograft mouse model following oral dosing.

Published

2020

19. Achieving

Author

Benjamin R, Bellenie, Kwai-Ming J, Cheung, Ana, Varela, Olivier A, Pierrat, Gavin W, Collie, Gary M, Box, Michael D, Bright, Sharon, Gowan, Angela, Hayes, Matthew J, Rodrigues, Kartika N, Shetty, Michael, Carter, Owen A, Davis, Alan T, Henley, Paolo, Innocenti, Louise D, Johnson, Manjuan, Liu, Selby, de Klerk, Yann-Vaï, Le Bihan, Matthew G, Lloyd, P Craig, McAndrew, Erald, Shehu, Rachel, Talbot, Hannah L, Woodward, Rosemary, Burke, Vladimir, Kirkin, Rob L M, van Montfort, Florence I, Raynaud, Olivia W, Rossanese, and Swen, Hoelder

Subjects

Male, Mice, Inbred BALB C, Mice, SCID, Xenograft Model Antitumor Assays, Article, Protein Structure, Tertiary, Rats, Rats, Sprague-Dawley, Mice, Drug Delivery Systems, immune system diseases, hemic and lymphatic diseases, Cell Line, Tumor, Drug Discovery, Microsomes, Liver, Proto-Oncogene Proteins c-bcl-6, Animals, Humans, Benzimidazoles, Female

Abstract

Deregulation of the transcriptional repressor BCL6 enables tumorigenesis of germinal center B-cells, and hence BCL6 has been proposed as a therapeutic target for the treatment of diffuse large B-cell lymphoma (DLBCL). Herein we report the discovery of a series of benzimidazolone inhibitors of the protein–protein interaction between BCL6 and its co-repressors. A subset of these inhibitors were found to cause rapid degradation of BCL6, and optimization of pharmacokinetic properties led to the discovery of 5-((5-chloro-2-((3R,5S)-4,4-difluoro-3,5-dimethylpiperidin-1-yl)pyrimidin-4-yl)amino)-3-(3-hydroxy-3-methylbutyl)-1-methyl-1,3-dihydro-2H-benzo[d]imidazol-2-one (CCT369260), which reduces BCL6 levels in a lymphoma xenograft mouse model following oral dosing.

Published

2020

20. Introduction of a Methyl Group Curbs Metabolism of Pyrido[3,4-d]pyrimidine Monopolar Spindle 1 (MPS1) Inhibitors and Enables the Discovery of the Phase 1 Clinical Candidate N2-(2-Ethoxy-4-(4-methyl-4H-1,2,4-triazol-3-yl)phenyl)-6-methyl-N8-neopentylpyrido[3,4-d]pyrimidine-2,8-diamine (BOS172722)

Author

Swen Hoelder, Rob L. M. van Montfort, Angela Hayes, Florence I. Raynaud, Suzanne A. Eccles, Amir Faisal, Jennie Roberts, Grace Mak, Melanie Valenti, Lisa O’Fee, Isaac M. Westwood, Alan T. Henley, Paolo Innocenti, Michael Carter, Hannah Woodward, Harry Saville, Gary Box, Fabio Broccatelli, Kwai-Ming J. Cheung, Julian Blagg, Nora Cronin, Alexis De Haven Brandon, Spiros Linardopoulos, Rosemary Burke, and Jessica Schmitt

Subjects

0301 basic medicine, Pyrimidine, Drug discovery, Stereochemistry, Methylation, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, 030220 oncology & carcinogenesis, Drug Discovery, Lipophilicity, Alkoxy group, Molecular Medicine, Structure–activity relationship, Pharmacophore, Methyl group

Abstract

Monopolar spindle 1 (MPS1) occupies a central role in mitosis and is one of the main components of the spindle assembly checkpoint. The MPS1 kinase is an attractive cancer target, and herein, we report the discovery of the clinical candidate BOS172722. The starting point for our work was a series of pyrido[3,4-d]pyrimidine inhibitors that demonstrated excellent potency and kinase selectivity but suffered from rapid turnover in human liver microsomes (HLM). Optimizing HLM stability proved challenging since it was not possible to identify a consistent site of metabolism and lowering lipophilicity proved unsuccessful. Key to overcoming this problem was the finding that introduction of a methyl group at the 6-position of the pyrido[3,4-d]pyrimidine core significantly improved HLM stability. Met ID studies suggested that the methyl group suppressed metabolism at the distant aniline portion of the molecule, likely by blocking the preferred pharmacophore through which P450 recognized the compound. This work ulti...

Published

2018

21. Correction

Author

Swee Y, Sharp, Kathy, Boxall, Martin, Rowlands, Chrisostomos, Prodromou, S Mark, Roe, Alison, Maloney, Marissa, Powers, Paul A, Clarke, Gary, Box, Sharon, Sanderson, Lisa, Patterson, Thomas P, Matthews, Kwai-Ming J, Cheung, Karen, Ball, Angela, Hayes, Florence, Raynaud, Richard, Marais, Laurence, Pearl, Sue, Eccles, Wynne, Aherne, Edward, McDonald, and Paul, Workman

Published

2019

22. Introduction of a Methyl Group Curbs Metabolism of Pyrido[3,4- d]pyrimidine Monopolar Spindle 1 (MPS1) Inhibitors and Enables the Discovery of the Phase 1 Clinical Candidate N

Author

Hannah L, Woodward, Paolo, Innocenti, Kwai-Ming J, Cheung, Angela, Hayes, Jennie, Roberts, Alan T, Henley, Amir, Faisal, Grace Wing-Yan, Mak, Gary, Box, Isaac M, Westwood, Nora, Cronin, Michael, Carter, Melanie, Valenti, Alexis, De Haven Brandon, Lisa, O'Fee, Harry, Saville, Jessica, Schmitt, Rosemary, Burke, Fabio, Broccatelli, Rob L M, van Montfort, Florence I, Raynaud, Suzanne A, Eccles, Spiros, Linardopoulos, Julian, Blagg, and Swen, Hoelder

Subjects

Male, Models, Molecular, Clinical Trials, Phase I as Topic, Molecular Structure, Protein Conformation, Cell Cycle Proteins, Protein Serine-Threonine Kinases, Protein-Tyrosine Kinases, Triazoles, Methylation, Article, Rats, Rats, Sprague-Dawley, Mice, Structure-Activity Relationship, Pyrimidines, Drug Discovery, Microsomes, Liver, Animals, Humans, Female, Tissue Distribution, Protein Kinase Inhibitors, Cells, Cultured

Abstract

Monopolar spindle 1 (MPS1) occupies a central role in mitosis and is one of the main components of the spindle assembly checkpoint. The MPS1 kinase is an attractive cancer target, and herein, we report the discovery of the clinical candidate BOS172722. The starting point for our work was a series of pyrido[3,4- d]pyrimidine inhibitors that demonstrated excellent potency and kinase selectivity but suffered from rapid turnover in human liver microsomes (HLM). Optimizing HLM stability proved challenging since it was not possible to identify a consistent site of metabolism and lowering lipophilicity proved unsuccessful. Key to overcoming this problem was the finding that introduction of a methyl group at the 6-position of the pyrido[3,4- d]pyrimidine core significantly improved HLM stability. Met ID studies suggested that the methyl group suppressed metabolism at the distant aniline portion of the molecule, likely by blocking the preferred pharmacophore through which P450 recognized the compound. This work ultimately led to the discovery of BOS172722 as a Phase 1 clinical candidate.

Published

2018

23. Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance

Author

Amir Faisal, Kwai-Ming J. Cheung, Julian Blagg, Grace Mak, Amy Wood, Swen Hoelder, Paul Workman, Craig McAndrew, Kathy Boxall, Mark D. Gurden, Rob L. M. van Montfort, Spiros Linardopoulos, Jessica Schmitt, Sébastien Naud, Rosemary Burke, and Isaac M. Westwood

Subjects

Models, Molecular, Cancer Research, Cell Survival, medicine.medical_treatment, Cell Cycle Proteins, Drug resistance, Protein Serine-Threonine Kinases, Pharmacology, Biology, medicine.disease_cause, Heterocyclic Compounds, 2-Ring, Targeted therapy, Gefitinib, Cell Line, Tumor, Neoplasms, medicine, Humans, Point Mutation, Protein Kinase Inhibitors, EGFR inhibitors, Mutation, Aniline Compounds, Dose-Response Relationship, Drug, Molecular Structure, Point mutation, Cancer, Protein-Tyrosine Kinases, HCT116 Cells, medicine.disease, Protein Structure, Tertiary, ErbB Receptors, HEK293 Cells, Oncology, Drug Resistance, Neoplasm, Cancer cell, Quinazolines, Cancer research, Pyrazoles, Protein Binding, medicine.drug

Abstract

Acquired resistance to therapy is perhaps the greatest challenge to effective clinical management of cancer. With several inhibitors of the mitotic checkpoint kinase MPS1 in preclinical development, we sought to investigate how resistance against these inhibitors may arise so that mitigation or bypass strategies could be addressed as early as possible. Toward this end, we modeled acquired resistance to the MPS1 inhibitors AZ3146, NMS-P715, and CCT251455, identifying five point mutations in the kinase domain of MPS1 that confer resistance against multiple inhibitors. Structural studies showed how the MPS1 mutants conferred resistance by causing steric hindrance to inhibitor binding. Notably, we show that these mutations occur in nontreated cancer cell lines and primary tumor specimens, and that they also preexist in normal lymphoblast and breast tissues. In a parallel piece of work, we also show that the EGFR p.T790M mutation, the most common mutation conferring resistance to the EGFR inhibitor gefitinib, also preexists in cancer cells and normal tissue. Our results therefore suggest that mutations conferring resistance to targeted therapy occur naturally in normal and malignant cells and these mutations do not arise as a result of the increased mutagenic plasticity of cancer cells. Cancer Res; 75(16); 3340–54. ©2015 AACR.

Published

2015

24. Multiparameter Lead Optimization to Give an Oral Checkpoint Kinase 1 (CHK1) Inhibitor Clinical Candidate: (R)-5-((4-((Morpholin-2-ylmethyl)amino)-5-(trifluoromethyl)pyridin-2-yl)amino)pyrazine-2-carbonitrile (CCT245737)

Author

Suzanne A. Eccles, Alexis De Haven Brandon, Yann Jamin, Isaac M. Westwood, Nathan J. Brown, Kwai-Ming J. Cheung, Nicolas Proisy, Michelle D. Garrett, Michael I. Walton, G. Wynne Aherne, Melanie Valenti, Rob L. M. van Montfort, K. Boxall, James Osborne, Gary Box, John C. Reader, Simon P. Robinson, Michael Lainchbury, Philip Leonard, Alan T. Henley, Florence I. Raynaud, Angela Hayes, Ian Collins, Thomas P. Matthews, T. McHardy, Marieke Lamers, and Paul D. Eve

Subjects

Models, Molecular, 0301 basic medicine, Stereochemistry, hERG, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Drug Discovery, Humans, Structure–activity relationship, CHEK1, 4-Aminopyridine, Protein Kinase Inhibitors, Trifluoromethyl, Dose-Response Relationship, Drug, Molecular Structure, biology, Chemistry, Potentiator, 030104 developmental biology, Biochemistry, Pyrazines, 030220 oncology & carcinogenesis, Checkpoint Kinase 1, Lipophilicity, biology.protein, Molecular Medicine, Adenosine triphosphate

Abstract

Multiparameter optimization of a series of 5-((4-aminopyridin-2-yl)amino)pyrazine-2-carbonitriles resulted in the identification of a potent and selective oral CHK1 preclinical development candidate with in vivo efficacy as a potentiator of deoxyribonucleic acid (DNA) damaging chemotherapy and as a single agent. Cellular mechanism of action assays were used to give an integrated assessment of compound selectivity during optimization resulting in a highly CHK1 selective adenosine triphosphate (ATP) competitive inhibitor. A single substituent vector directed away from the CHK1 kinase active site was unexpectedly found to drive the selective cellular efficacy of the compounds. Both CHK1 potency and off-target human ether-a-go-go-related gene (hERG) ion channel inhibition were dependent on lipophilicity and basicity in this series. Optimization of CHK1 cellular potency and in vivo pharmacokinetic-pharmacodynamic (PK-PD) properties gave a compound with low predicted doses and exposures in humans which mitigated the residual weak in vitro hERG inhibition.

Published

2016

25. Design of Potent and Selective Hybrid Inhibitors of the Mitotic Kinase Nek2: Structure–Activity Relationship, Structural Biology, and Cellular Activity

Author

Kwai-Ming J. Cheung, Joanne E. Baxter, Andrew M. Fry, K. Boxall, Savade Solanki, Swen Hoelder, Tara Hardy, Paolo Innocenti, Lisa Pickard, Fiona C. Rowan, Corine Mas-Droux, G.W. Aherne, Maura Westlake, Richard Bayliss, and Sharon Yeoh

Subjects

Protein-Serine-Threonine Kinases, Structural biology, Biochemistry, Chemistry, Drug Discovery, Molecular Medicine, Structure–activity relationship, Transferase, Phosphorylation, Stereoisomerism, NIMA-Related Kinases, Mitosis

Abstract

We report herein a series of Nek2 inhibitors based on an aminopyridine scaffold. These compounds have been designed by combining key elements of two previously discovered chemical series. Structure based design led to aminopyridine (R)-21, a potent and selective inhibitor able to modulate Nek2 activity in cells.

Published

2012

26. Structure-Guided Evolution of Potent and Selective CHK1 Inhibitors through Scaffold Morphing

Author

Alexis De Haven Brandon, Glynn Addison, Suzanne A. Eccles, Suzanne Taylor, Michelle D. Garrett, Ian Collins, Thomas P. Matthews, Nicolas Proisy, Angela Hayes, Rob L. M. van Montfort, John M. Ellard, Michael I. Walton, Nelly Piton, Samantha Burns, John C. Reader, Kwai-Ming J. Cheung, Michael Cherry, Paul D. Eve, Isaac M. Westwood, Kathy Boxall, Gary Box, Florence I. Raynaud, Jane Elizabeth Scanlon, Melanie Valenti, G. Wynne Aherne, Suki Klair, Martin Fisher, and David Williams

Subjects

Scaffold, animal structures, Pyridines, Stereochemistry, Transplantation, Heterologous, Molecular Conformation, Biological Availability, Mice, Nude, Antineoplastic Agents, Stereoisomerism, Crystallography, X-Ray, Article, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Adenosine Triphosphate, In vivo, Cell Line, Tumor, Drug Discovery, Pyrazolopyridine, Animals, Humans, Structure–activity relationship, Isoquinoline, Protein Kinase Inhibitors, chemistry.chemical_classification, Binding Sites, Isoquinolines, Transplantation, chemistry, Pyrazines, Checkpoint Kinase 1, Molecular Medicine, Drug Screening Assays, Antitumor, biological phenomena, cell phenomena, and immunity, Protein Kinases, Neoplasm Transplantation, Tricyclic

Abstract

Pyrazolopyridine inhibitors with low micromolar potency for CHK1 and good selectivity against CHK2 were previously identified by fragment-based screening. The optimization of the pyrazolopyridines to a series of potent and CHK1-selective isoquinolines demonstrates how fragment-growing and scaffold morphing strategies arising from a structure-based understanding of CHK1 inhibitor binding can be combined to successfully progress fragment-derived hit matter to compounds with activity in vivo. The challenges of improving CHK1 potency and selectivity, addressing synthetic tractability, and achieving novelty in the crowded kinase inhibitor chemical space were tackled by multiple scaffold morphing steps, which progressed through tricyclic pyrimido[2,3-b]azaindoles to N-(pyrazin-2-yl)pyrimidin-4-amines and ultimately to imidazo[4,5-c]pyridines and isoquinolines. A potent and highly selective isoquinoline CHK1 inhibitor (SAR-020106) was identified, which potentiated the efficacies of irinotecan and gemcitabine in SW620 human colon carcinoma xenografts in nude mice.

Published

2011

27. Correction: In vitro Biological Characterization of a Novel, Synthetic Diaryl Pyrazole Resorcinol Class of Heat Shock Protein 90 Inhibitors

Author

Swee Y. Sharp, Kathy Boxall, Martin Rowlands, Chrisostomos Prodromou, S. Mark Roe, Alison Maloney, Marissa Powers, Paul A. Clarke, Gary Box, Sharon Sanderson, Lisa Patterson, Thomas P. Matthews, Kwai-Ming J. Cheung, Karen Ball, Angela Hayes, Florence Raynaud, Richard Marais, Laurence Pearl, Sue Eccles, Wynne Aherne, Edward McDonald, and Paul Workman

Subjects

Cancer Research, Oncology

Published

2019

28. A facile synthesis of pyrazoles with multi-point structural diversity by 1,3-dipolar cycloaddition

Author

Jóhannes Reynisson, Kwai Ming J. Cheung, and Edward McDonald

Subjects

chemistry.chemical_classification, Aryl, Organic Chemistry, Regioselectivity, Pyrazole, Biochemistry, Combinatorial chemistry, Cycloaddition, chemistry.chemical_compound, chemistry, Ethyl diazoacetate, Drug Discovery, 1,3-Dipolar cycloaddition, Structural isomer, Alkyl

Abstract

We describe the synthesis of diverse pyrazoles by 1,3-dipolar cycloaddition of ethyl diazoacetate with various acetylenes in refluxing toluene. The product pyrazoles are useful starting points for preparing a diverse collection of trisubstituted pyrazole carboxamides. For aryl and heteroaryl alkynes a single product is obtained while alkyl alkynes afford a ca. 6:1 mixture of regioisomers. The observed regioselectivity for the cycloaddition step and the ease of reaction are consistent with predictions derived from computing the HOMO–LUMO energies of the reactants.

Published

2010

29. Abstract 1651: In vitro and in vivo profile of the preclinical candidate and MPS1 kinase inhibitor CCT289346

Author

Amir Faisal, Paolo Innocenti, Harry Saville, Gary Box, Jennie Roberts, Kwai-Ming J. Cheung, Julian Blagg, Melanie Valenti, Angela Hayes, Grace Mak, Suzanne A. Eccles, Sébastien Naud, Katie Walsh, Lisa O’Fee, Alexis De Haven Brandon, Spiros Linardopoulos, Florence I. Raynaud, Rosemary Burke, Swen Hoelder, Rob L. M. van Montfort, Hannah Woodward, and Alan T. Heneley

Subjects

Cancer Research, Oncology, Chemistry, Kinase, In vivo, Pharmacology, In vitro

Abstract

The mitotic kinase MPS1 (also known as TTK) is one of the main components of the spindle assembly checkpoint. MPS1 is required for chromosome alignment and kinetochore-microtubule error correction. Cancer cells are dependent on MPS1 to cope with chromosomal instability resulting from aberrant numbers of chromosomes. Moreover, MPS1 has been found to be deregulated in a large number of tumor types. MPS1 kinase inhibitors induce cancer cells to prematurely exit mitosis with incorrectly attached and unaligned chromosomes, causing severe chromosome mis-segregation, aneuploidy and cell death. These data stimulated us to pursue MPS1 as a cancer target. Extensive work by us and other groups has shown that MPS1 inhibitors are effective against a variety of cancers, particularly when used in combination with other drugs, such as paclitaxel. Here we disclose CCT289346, an MPS1 inhibitor currently completing late stage preclinical development. We describe the final stages of chemical optimisation and the data driven selection and nomination of CCT289346 as our preclinical candidate. We report key in vitro and in vivo preclinical data such as kinase profiling, PK in mouse, rat and dog, PK/PD relationship and efficacy in different in vivo models. Citation Format: Hannah Woodward, Paolo Innocenti, Kwai-Ming J. Cheung, Sébastien Naud, Amir Faisal, Grace W. Mak, Angela Hayes, Lisa O'Fee, Harry Saville, Alexis De Haven Brandon, Jennie Roberts, Gary Box, Melanie Valenti, Alan T. Heneley, Katie Walsh, Rosemary Burke, Suzanne A. Eccles, Florence I. Raynaud, Rob L. van Montfort, Julian Blagg, Spiros Linardopoulos, Swen Hoelder. In vitro and in vivo profile of the preclinical candidate and MPS1 kinase inhibitor CCT289346 [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 1651.

Published

2018

30. 4,5-Diarylisoxazole Hsp90 Chaperone Inhibitors: Potential Therapeutic Agents for the Treatment of Cancer

Author

Karen James, Ian Collins, Kathy Boxall, Brian Dymock, Paul Workman, Florence I. Raynaud, Chrisostomos Prodromou, Angela Hayes, Suzanne A. Eccles, Kwai-Ming J. Cheung, Allan E. Surgenor, Paul Webb, Martin J. Drysdale, D. Lee Walmsley, Stuart C. Ray, Allan M. Jordan, Jenifer Borgognoni, Vanessa Martins, Swee Y. Sharp, Andrea M. Lockie, Nicholas G. M. Davies, R. Howes, Lisa Wright, Thomas P. Matthews, Andrew Massey, Michael Wood, Roderick E. Hubbard, Wynne Aherne, Stephen D. Roughley, Alexandra Fink, Harry Finch, Julie E. Cansfield, Christopher J. Northfield, Paul Brough, Edward McDonald, Xavier Barril, and Laurence H. Pearl

Subjects

Models, Molecular, Transplantation, Heterologous, Mice, Nude, Antineoplastic Agents, Fluorescence Polarization, Crystallography, X-Ray, Binding, Competitive, Mice, Structure-Activity Relationship, In vivo, Cell Line, Tumor, Drug Discovery, Animals, Humans, Structure–activity relationship, HSP90 Heat-Shock Proteins, Cell Proliferation, biology, Cell growth, Chemistry, Ligand binding assay, Isoxazoles, Resorcinols, Hsp90, In vitro, Transplantation, Biochemistry, Cancer research, biology.protein, Molecular Medicine, Drug Screening Assays, Antitumor, Signal transduction, Neoplasm Transplantation

Abstract

Inhibitors of the Hsp90 molecular chaperone are showing considerable promise as potential chemotherapeutic agents for cancer. Here, we describe the structure-based design, synthesis, structure-activity relationships and pharmacokinetics of potent small-molecule inhibitors of Hsp90 based on the 4,5-diarylisoxazole scaffold. Analogues from this series have high affinity for Hsp90, as measured in a fluorescence polarization (FP) competitive binding assay, and are active in cancer cell lines where they inhibit proliferation and exhibit a characteristic profile of depletion of oncogenic proteins and concomitant elevation of Hsp72. Compound 40f (VER-52296/NVP-AUY922) is potent in the Hsp90 FP binding assay (IC50 = 21 nM) and inhibits proliferation of various human cancer cell lines in vitro, with GI50 averaging 9 nM. Compound 40f is retained in tumors in vivo when administered i.p., as evaluated by cassette dosing in tumor-bearing mice. In a human colon cancer xenograft model, 40f inhibits tumor growth by approximately 50%.

Published

2007

31. Abstract 193: Inhibitors of MPS1: Discovery of CCT289346, a highly potent, selective and orally available preclinical candidate

Author

Lisa O’Fee, Angela Hayes, Rob L. M. van Montfort, Swen Hoelder, Sébastien Naud, Suzanne A. Eccles, Florence I. Raynaud, Hannah Woodward, Kwai-Ming J. Cheung, Julian Blagg, Isaac M. Westwood, Grace Mak, Alexis De Haven Brandon, Spiros Linardopoulos, Alan T. Henley, Paolo Innocenti, Rosemary Burke, Harry Saville, Gary Box, Michael Carter, Amir Faisal, and Melanie Valenti

Subjects

Cancer Research, Human liver, Kinase, Cancer, Biology, medicine.disease, Oncology, In vivo, Cancer cell, Cancer research, medicine, Protein kinase A, Monopolar spindle, ADME

Abstract

MPS1 (also known as TTK), is a dual-specificity protein kinase and one of the main components of the spindle assembly checkpoint. Cancer cells heavily rely on MPS1 to cope with aneuploidy resulting from aberrant numbers of chromosomes and MPS1 has been found to be upregulated in a large number of tumor types. Extensive work by us and other groups has shown that MPS1 inhibitors are effective against a variety of cancers, particularly when used in combination with other drugs, for example, tubulin-targeting agents. We recently reported the structure-based design and discovery of a series of pyrido[3,4-d]pyrimidines inhibitors of MPS1 (1). Advanced compounds showed very potent inhibition of MPS1 in biochemical and cellular assays. However, these compounds suffered from high lipophilicity and pronounced metabolism in human liver microsomes preventing progression into preclinical development. Here we report the optimisation of this series ultimately yielding CCT289346, our preclinical candidate. CCT289346 shows excellent potency, kinase selectivity, and ADME properties including stability in human liver microsomes. The compound has been produced on a kilogram scale and is currently undergoing preclinical development. We will discuss our design approach and hypotheses leading to the discovery of CCT289346 and disclose in vivo efficacy data. References 1. Innocenti P et al. Rapid Discovery of Pyrido[3,4-d]pyrimidine Inhibitors of Monopolar Spindle Kinase 1 (MPS1) Using a Structure-Based Hybridization Approach. Journal of Medicinal Chemistry. 2016; 59(8):3671-88. Citation Format: Hannah L. Woodward, Paolo Innocenti, Kwai-Ming J. Cheung, Sébastien Naud, Angela Hayes, Alan T. Henley, Amir Faisal, Grace Mak, Gary Box, Isaac M. Westwood, Michael Carter, Melanie Valenti, Alexis De Haven Brandon, Lisa O’Fee, Harry Saville, Rosemary Burke, Rob van Montfort, Florence Raynaud, Suzanne A. Eccles, Spiros Linardopoulos, Julian Blagg, Swen Hoelder. Inhibitors of MPS1: Discovery of CCT289346, a highly potent, selective and orally available preclinical candidate [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 193. doi:10.1158/1538-7445.AM2017-193

Published

2017

32. Structure-based design of orally bioavailable 1H-pyrrolo[3,2-c]pyridine inhibitors of mitotic kinase monopolar spindle 1 (MPS1)

Author

Amir Faisal, Kwai-Ming J. Cheung, Peter Sheldrake, Julian Blagg, Manjuan Liu, Isaac M. Westwood, Craig McAndrew, Grace Mak, Kathy Boxall, Vanessa Choi, Florence I. Raynaud, Amy Wood, Alan T. Henley, Angela Hayes, Rob L. M. van Montfort, Ross Baker, Swen Hoelder, Melanie Valenti, Alexis De Haven Brandon, Spiros Linardopoulos, Rosemary Burke, Vassilios Bavetsias, Mark D. Gurden, Berry Matijssen, Suzanne A. Eccles, Butrus Atrash, Jessica Schmitt, and Sébastien Naud

Subjects

Models, Molecular, Administration, Oral, Biological Availability, Cell Cycle Proteins, Protein Serine-Threonine Kinases, Heterocyclic Compounds, 2-Ring, Article, Structure-Activity Relationship, Chromosome instability, Drug Discovery, Structure–activity relationship, Transferase, Cell Cycle Protein, Protein kinase A, Gene, Protein Kinase Inhibitors, Protein-Serine-Threonine Kinases, Aniline Compounds, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Protein-Tyrosine Kinases, Spindle checkpoint, Biochemistry, Drug Design, Cancer research, Molecular Medicine

Abstract

The protein kinase MPS1 is a crucial component of the spindle assembly checkpoint signal and is aberrantly overexpressed in many human cancers. MPS1 is one of the top 25 genes overexpressed in tumors with chromosomal instability and aneuploidy. PTEN-deficient breast tumor cells are particularly dependent upon MPS1 for their survival, making it a target of significant interest in oncology. We report the discovery and optimization of potent and selective MPS1 inhibitors based on the 1H-pyrrolo[3,2-c]pyridine scaffold, guided by structure-based design and cellular characterization of MPS1 inhibition, leading to 65 (CCT251455). This potent and selective chemical tool stabilizes an inactive conformation of MPS1 with the activation loop ordered in a manner incompatible with ATP and substrate-peptide binding; it displays a favorable oral pharmacokinetic profile, shows dose-dependent inhibition of MPS1 in an HCT116 human tumor xenograft model, and is an attractive tool compound to elucidate further the therapeutic potential of MPS1 inhibition.

Published

2013

33. ChemInform Abstract: A Facile Synthesis of Pyrazoles with Multi-Point Structural Diversity by 1,3-Dipolar Cycloaddition

Author

Edward McDonald, Kwai Ming J. Cheung, and Jóhannes Reynisson

Subjects

Chemistry, Stereochemistry, 1,3-Dipolar cycloaddition, Structural isomer, Structural diversity, General Medicine, Cycloaddition, Multi point

Abstract

The cycloaddition of terminal alkynes with ester (II) affords the 3-substituted regioisomers as main or exclusive products.

Published

2011

34. Aminopyrazine inhibitors binding to an unusual inactive conformation of the mitotic kinase Nek2: SAR and structural characterization

Author

Swen Hoelder, Savade Solanki, Rob L. M. van Montfort, Douglas W. Thomson, Richard Bayliss, Caterina Barillari, Kwai-Ming J. Cheung, Daniel K. Whelligan, Corine Mas-Droux, Kathy Boxall, Dawn Taylor, Charles G. Grummitt, Ian Collins, G. Wynne Aherne, and Samantha Burns

Subjects

Models, Molecular, Protein-Serine-Threonine Kinases, Kinase, Chemistry, Stereochemistry, Protein Conformation, Stereoisomerism, Plasma protein binding, Protein Serine-Threonine Kinases, Crystallography, X-Ray, Article, Structure-Activity Relationship, Protein structure, Structural biology, Biochemistry, Pyrazines, Drug Discovery, Molecular Medicine, Transferase, Structure–activity relationship, Humans, NIMA-Related Kinases, Phosphorylation, Protein Binding

Abstract

We report herein the first systematic exploration of inhibitors of the mitotic kinase Nek2. Starting from HTS hit aminopyrazine 2, compounds with improved activity were identified using structure-based design. Our structural biology investigations reveal two notable observations. First, 2 and related compounds bind to an unusual, inactive conformation of the kinase which to the best of our knowledge has not been reported for other types of kinase inhibitors. Second, a phenylalanine residue at the center of the ATP pocket strongly affects the ability of the inhibitor to bind to the protein. The implications of these observations are discussed, and the work described here defines key features for potent and selective Nek2 inhibition, which will aid the identification of more advanced inhibitors of Nek2.

Published

2010

35. Identification of inhibitors of checkpoint kinase 1 through template screening

Author

Ian Collins, Michael Cherry, Kathy Boxall, Martin Fisher, Samantha Burns, David Williams, Kwai-Ming J. Cheung, G. Wynne Aherne, Isaac M. Westwood, T. McHardy, John C. Reader, Thomas P. Matthews, Suki Klair, Michael I. Walton, Rob L. M. van Montfort, and Michelle D. Garrett

Subjects

Cell cycle checkpoint, Ligand efficiency, Chemistry, In silico, Drug Evaluation, Preclinical, Hydrogen Bonding, Small molecule, Structure-Activity Relationship, Biochemistry, Structural biology, Drug Discovery, Pyrazolopyridine, Checkpoint Kinase 1, Molecular Medicine, Structure–activity relationship, Humans, CHEK1, HT29 Cells, Protein Kinase Inhibitors, Protein Kinases

Abstract

Checkpoint kinase 1 (CHK1) is an oncology target of significant current interest. Inhibition of CHK1 abrogates DNA damage-induced cell cycle checkpoints and sensitizes p53 deficient cancer cells to genotoxic therapies. Using template screening, a fragment-based approach to small molecule hit generation, we have identified multiple CHK1 inhibitor scaffolds suitable for further optimization. The sequential combination of in silico low molecular weight template selection, a high concentration biochemical assay and hit validation through protein-ligand X-ray crystallography provided 13 template hits from an initial in silico screening library of ca. 15000 compounds. The use of appropriate counter-screening to rule out nonspecific aggregation by test compounds was essential for optimum performance of the high concentration bioassay. One low molecular weight, weakly active purine template hit was progressed by iterative structure-based design to give submicromolar pyrazolopyridines with good ligand efficiency and appropriate CHK1-mediated cellular activity in HT29 colon cancer cells.

Published

2009

36. Inhibition of the heat shock protein 90 molecular chaperone in vitro and in vivo by novel, synthetic, potent resorcinylic pyrazole/isoxazole amide analogues

Author

Gary Box, Allan E. Surgenor, Kwai-Ming J. Cheung, Keith Jones, Marissa V. Powers, Laurence H. Pearl, Nicolas Foloppe, Swee Y. Sharp, Wynne Aherne, Lisa Wright, Brian Dymock, Paul Brough, Karen James, Anthea Hardcastle, Andrew Kalusa, Xavier Barril, Joanna L. Holmes, Chrisostomos Prodromou, Paul Workman, Sue Eccles, Martin J. Drysdale, Edward McDonald, Roderick E. Hubbard, Julie E. Cansfield, Kathy Boxall, Florence I. Raynaud, Angela Hayes, and Thomas P. Matthews

Subjects

Cancer Research, genetic structures, Mice, Nude, Apoptosis, Biology, Pyrazole, Crystallography, X-Ray, chemistry.chemical_compound, Mice, Heat shock protein, NAD(P)H Dehydrogenase (Quinone), Animals, Humans, HSP90 Heat-Shock Proteins, Isoxazole, Cell Proliferation, Adenosine Triphosphatases, Cell Cycle, Endothelial Cells, Isoxazoles, HCT116 Cells, Hsp90, Xenograft Model Antitumor Assays, eye diseases, Dissociation constant, Treatment Outcome, Oncology, Biochemistry, chemistry, Drug Resistance, Neoplasm, biology.protein, Pyrazoles, Female, NAD+ kinase, Growth inhibition, HT29 Cells, Biomarkers, Protein Binding

Abstract

Although the heat shock protein 90 (HSP90) inhibitor 17-allylamino-17-demethoxygeldanamycin (17-AAG) shows clinical promise, potential limitations encourage development of alternative chemotypes. We discovered the 3,4-diarylpyrazole resorcinol CCT018159 by high-throughput screening and used structure-based design to generate more potent pyrazole amide analogues, exemplified by VER-49009. Here, we describe the detailed biological properties of VER-49009 and the corresponding isoxazole VER-50589. X-ray crystallography showed a virtually identical HSP90 binding mode. However, the dissociation constant (Kd) of VER-50589 was 4.5 ± 2.2 nmol/L compared with 78.0 ± 10.4 nmol/L for VER-49009, attributable to higher enthalpy for VER-50589 binding. A competitive binding assay gave a lower IC50 of 21 ± 4 nmol/L for VER-50589 compared with 47 ± 9 nmol/L for VER-49009. Cellular uptake of VER-50589 was 4-fold greater than for VER-49009. Mean cellular antiproliferative GI50 values for VER-50589 and VER-49009 for a human cancer cell line panel were 78 ± 15 and 685 ± 119 nmol/L, respectively, showing a 9-fold potency gain for the isoxazole. Unlike 17-AAG, but as with CCT018159, cellular potency of these analogues was independent of NAD(P)H:quinone oxidoreductase 1/DT-diaphorase and P-glycoprotein expression. Consistent with HSP90 inhibition, VER-50589 and VER-49009 caused induction of HSP72 and HSP27 alongside depletion of client proteins, including C-RAF, B-RAF, and survivin, and the protein arginine methyltransferase PRMT5. Both caused cell cycle arrest and apoptosis. Extent and duration of pharmacodynamic changes in an orthotopic human ovarian carcinoma model confirmed the superiority of VER-50589 over VER-49009. VER-50589 accumulated in HCT116 human colon cancer xenografts at levels above the cellular GI50 for 24 h, resulting in 30% growth inhibition. The results indicate the therapeutic potential of the resorcinylic pyrazole/isoxazole amide analogues as HSP90 inhibitors. [Mol Cancer Ther 2007;6(4):1198–211]

Published

2007

37. In vitro biological characterization of a novel, synthetic diaryl pyrazole resorcinol class of heat shock protein 90 inhibitors

Author

Chrisostomos Prodromou, Angela Hayes, Kwai-Ming J. Cheung, Sharon Sanderson, Paul A. Clarke, Richard Marais, Karen Ball, Marissa V. Powers, Paul Workman, Sue Eccles, Swee Y. Sharp, Wynne Aherne, Edward McDonald, Kathy Boxall, S. Mark Roe, Lisa Patterson, Martin G. Rowlands, Alison Maloney, Gary Box, Florence I. Raynaud, Laurence H. Pearl, and Thomas P. Matthews

Subjects

Models, Molecular, Cancer Research, Apoptosis, Biology, Pyrazole, Crystallography, X-Ray, Heterocyclic Compounds, 2-Ring, Models, Biological, Hsp90 inhibitor, Substrate Specificity, chemistry.chemical_compound, Heat shock protein, polycyclic compounds, Tumor Cells, Cultured, Humans, HSP90 Heat-Shock Proteins, Cell Proliferation, Adenosine Triphosphatases, Cell Cycle, Geldanamycin, Cytostasis, Hsp90, In vitro, Radicicol, Oncology, Biochemistry, chemistry, Drug Resistance, Neoplasm, biology.protein, Pyrazoles, Protein Binding

Abstract

The molecular chaperone heat shock protein 90 (HSP90) has emerged as an exciting molecular target. Derivatives of the natural product geldanamycin, such as 17-allylamino-17-demethoxy-geldanamycin (17-AAG), were the first HSP90 ATPase inhibitors to enter clinical trial. Synthetic small-molecule HSP90 inhibitors have potential advantages. Here, we describe the biological properties of the lead compound of a new class of 3,4-diaryl pyrazole resorcinol HSP90 inhibitor (CCT018159), which we identified by high-throughput screening. CCT018159 inhibited human HSP90β with comparable potency to 17-AAG and with similar ATP-competitive kinetics. X-ray crystallographic structures of the NH2-terminal domain of yeast Hsp90 complexed with CCT018159 or its analogues showed binding properties similar to radicicol. The mean cellular GI50 value of CCT018159 across a panel of human cancer cell lines, including melanoma, was 5.3 μmol/L. Unlike 17-AAG, the in vitro antitumor activity of the pyrazole resorcinol analogues is independent of NQO1/DT-diaphorase and P-glycoprotein expression. The molecular signature of HSP90 inhibition, comprising increased expression of HSP72 protein and depletion of ERBB2, CDK4, C-RAF, and mutant B-RAF, was shown by Western blotting and quantified by time-resolved fluorescent-Cellisa in human cancer cell lines treated with CCT018159. CCT018159 caused cell cytostasis associated with a G1 arrest and induced apoptosis. CCT018159 also inhibited key endothelial and tumor cell functions implicated in invasion and angiogenesis. Overall, we have shown that diaryl pyrazole resorcinols exhibited similar cellular properties to 17-AAG with potential advantages (e.g., aqueous solubility, independence from NQO1 and P-glycoprotein). These compounds form the basis for further structure-based optimization to identify more potent inhibitors suitable for clinical development. [Cancer Res 2007;67(5):2206–16]

Published

2007

38. The identification, synthesis, protein crystal structure and in vitro biochemical evaluation of a new 3,4-diarylpyrazole class of Hsp90 inhibitors

Author

Kwai-Ming J. Cheung, K. Boxall, Chrisostomos Prodromou, S. Mark Roe, Laurence H. Pearl, Martin G. Rowlands, Swee Y. Sharp, Thomas P. Matthews, Edward McDonald, Karen James, G. Wynne Aherne, Paul Workman, and Alison Maloney

Subjects

Models, Molecular, Molecular model, Stereochemistry, Protein Conformation, ATPase, Clinical Biochemistry, Molecular Conformation, Pharmaceutical Science, Crystallography, X-Ray, Biochemistry, Chemical synthesis, Heterocyclic Compounds, 2-Ring, Structure-Activity Relationship, Protein structure, Cell Line, Tumor, Yeasts, Drug Discovery, Structure–activity relationship, Humans, HSP90 Heat-Shock Proteins, Enzyme Inhibitors, Molecular Biology, Cell Proliferation, Adenosine Triphosphatases, biology, Chemistry, Organic Chemistry, Hydrogen Bonding, Hsp90, Structural biology, Enzyme inhibitor, Drug Design, biology.protein, Molecular Medicine, Pyrazoles

Abstract

High-throughput screening identified the 3,4-diarylpyrazole CCT018159 as a novel and potent (7.1 microM) inhibitor of Hsp90 ATPase activity. Here, we describe the synthesis of CCT018159 and a number of close analogues together with data on their biochemical properties. Some initial structure-activity relationships are discussed, as well as the crystal structure of CCT018159 bound to Hsp90.

Published

2005

39. Identification of Inhibitors of Checkpoint Kinase 1 through Template Screening.

Author

Thomas P. Matthews, Suki Klair, Samantha Burns, Kathy Boxall, Michael Cherry, Martin Fisher, Isaac M. Westwood, Michael I. Walton, Tatiana McHardy, Kwai-Ming J. Cheung, Rob Van Montfort, David Williams, G. Wynne Aherne, Michelle D. Garrett, John Reader, and Ian Collins

Published

2009

40. 4,5-Diarylisoxazole Hsp90 Chaperone Inhibitors: Potential Therapeutic Agents for the Treatment of Cancer.

Author

Paul A. Brough, Wynne Aherne, Xavier Barril, Jenifer Borgognoni, Kathy Boxall, Julie E. Cansfield, Kwai-Ming J. Cheung, Ian Collins, Nicholas G. M. Davies, Martin J. Drysdale, Brian Dymock, Suzanne A. Eccles, Harry Finch, Alexandra Fink, Angela Hayes, Robert Howes, Roderick E. Hubbard, Karen James, Allan M. Jordan, and Andrea Lockie

Published

2007

41. Naturally Occurring Mutations in the MPS1 Gene Predispose Cells to Kinase Inhibitor Drug Resistance.

Author

Gurden, Mark D., Westwood, Isaac M., Faisal, Amir, Naud, Sébastien, Kwai-Ming J. Cheung, McAndrew, Craig, Wood, Amy, Schmitt, Jessica, Boxall, Kathy, Mak, Grace, Workman, Paul, Burke, Rosemary, Hoelder, Swen, Blagg, Julian, Van Montfort, Rob L. M., and Linardopoulos, Spiros

Subjects

*DRUG resistance in cancer cells, *KINASE inhibitors, *GENETIC mutation, *LYMPHOBLASTOID cell lines, *GEFITINIB, *THERAPEUTICS

Abstract

Acquired resistance to therapy is perhaps the greatest challenge to effective clinical management of cancer. With several inhibitors of the mitotic checkpoint kinase MPS1 in preclinical development, we sought to investigate how resistance against these inhibitors may arise so that mitigation or bypass strategies could be addressed as early as possible. Toward this end, we modeled acquired resistance to the MPS1 inhibitors AZ3146, NMS-P715, and CCT251455, identifying five point mutations in the kinase domain of MPS1 that confer resistance against multiple inhibitors. Structural studies showed how the MPS1 mutants conferred resistance by causing steric hindrance to inhibitor binding. Notably, we show that these mutations occur in nontreated cancer cell lines and primary tumor specimens, and that they also preexist in normal lymphoblast and breast tissues. In a parallel piece of work, we also show that the EGFR p.T790M mutation, the most common mutation conferring resistance to the EGFR inhibitor gefitinib, also preexists in cancer cells and normal tissue. Our results therefore suggest that mutations conferring resistance to targeted therapy occur naturally in normal and malignant cells and these mutations do not arise as a result of the increased mutagenic plasticity of cancer cells. [ABSTRACT FROM AUTHOR]

Published

2015