Your search keyword '"Joost C.M. Uitdehaag"' showing total 80 results

1. Structural insights into human Arginase-1 pH dependence and its inhibition by the small molecule inhibitor CB-1158

Author

Yvonne Grobben, Joost C.M. Uitdehaag, Nicole Willemsen-Seegers, Werner W.A. Tabak, Jos de Man, Rogier C. Buijsman, and Guido J.R. Zaman

Subjects

Cancer immunotherapy, Biochemical inhibition, Surface plasmon resonance, Thermal stability, X-ray crystallography, Biology (General), QH301-705.5

Abstract

Arginase-1 is a manganese-dependent metalloenzyme that catalyzes the hydrolysis of L-arginine into L-ornithine and urea. Arginase-1 is abundantly expressed by tumor-infiltrating myeloid cells that promote tumor immunosuppression, which is relieved by inhibition of Arginase-1. We have characterized the potencies of the Arginase-1 reference inhibitors (2S)-2-amino-6-boronohexanoic acid (ABH) and Nω-hydroxy-nor-L-arginine (nor-NOHA), and studied their pH-dependence and binding kinetics. To gain a better understanding of the structural changes underlying the high pH optimum of Arginase-1 and its pH-dependent inhibition, we determined the crystal structure of the human Arginase-1/ABH complex at pH 7.0 and 9.0. These structures revealed that at increased pH, the manganese cluster assumes a more symmetrical coordination structure, which presumably contributes to its increase in catalytic activity. Furthermore, we show that binding of ABH involves the presence of a sodium ion close to the manganese cluster. We also studied the investigational new drug CB-1158 (INCB001158). This inhibitor has a low-nanomolar potency at pH 7.4 and increases the thermal stability of Arginase-1 more than ABH and nor-NOHA. Moreover, CB-1158 displays slow association and dissociation kinetics at both pH 9.5 and 7.4, as indicated by surface plasmon resonance. The potent character of CB-1158 is presumably due to its increased rigidity compared to ABH as well as the formation of an additional hydrogen-bond network as observed by resolution of the Arginase-1/CB-1158 crystal structure.

Published

2020

2. Structural modeling of JAK1 mutations in T-cell acute lymphoblastic leukemia reveals a second contact site between pseudokinase and kinase domains

Author

Kirsten Canté-Barrett, Joost C.M. Uitdehaag, and Jules P.P. Meijerink

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Published

2016

3. Supplementary Table S4 from Combined Cellular and Biochemical Profiling to Identify Predictive Drug Response Biomarkers for Kinase Inhibitors Approved for Clinical Use between 2013 and 2017

Author

Guido J.R. Zaman, Rogier C. Buijsman, Suzanne J.C. van Gerwen, Jos de Man, Masaaki Sawa, Yusuke Kawase, Nicole Willemsen-Seegers, Jelle Dylus, Martine B.W. Prinsen, Jeroen A.D.M. de Roos, Jeffrey J. Kooijman, and Joost C.M. Uitdehaag

Abstract

Validation of predictive response biomarkers

Published

2023

4. Supplementary Table S2 from Cell Panel Profiling Reveals Conserved Therapeutic Clusters and Differentiates the Mechanism of Action of Different PI3K/mTOR, Aurora Kinase and EZH2 Inhibitors

Author

Guido J.R. Zaman, Rogier C. Buijsman, Jos de Man, Suzanne J.C. van Gerwen, Masaaki Sawa, Jeffrey Kooijman, Antoon M. van Doornmalen, Jelle Dylus, Judith R.F. de Vetter, Nicole Willemsen-Seegers, Martine B.W. Prinsen, Jeroen A.D.M. de Roos, and Joost C.M. Uitdehaag

Abstract

Structures of compounds used in the study

Published

2023

5. Table S2 from TTK Inhibitors as a Targeted Therapy for CTNNB1 (β-catenin) Mutant Cancers

Author

Joost C.M. Uitdehaag, Rogier C. Buijsman, Jos de Man, Martine B.W. Prinsen, Marion A.A. Libouban, Jeroen A.D.M. de Roos, and Guido J.R. Zaman

Abstract

Reanalyis of cell panel profilings of TTK inhibitors from literature

Published

2023

6. Data from TTK Inhibitors as a Targeted Therapy for CTNNB1 (β-catenin) Mutant Cancers

Author

Joost C.M. Uitdehaag, Rogier C. Buijsman, Jos de Man, Martine B.W. Prinsen, Marion A.A. Libouban, Jeroen A.D.M. de Roos, and Guido J.R. Zaman

Abstract

The spindle assembly checkpoint kinase TTK (Mps1) is a key regulator of chromosome segregation and is the subject of novel targeted therapy approaches by small-molecule inhibitors. Although the first TTK inhibitors have entered phase I dose escalating studies in combination with taxane chemotherapy, a patient stratification strategy is still missing. With the aim to identify a genomic biomarker to predict the response of tumor cells to TTK inhibitor therapy, we profiled a set of preclinical and clinical TTK inhibitors from different chemical series on a panel of 66 genetically characterized cell lines derived from different tumors (Oncolines). Cell lines harboring activating mutations in the CTNNB1 gene, encoding the Wnt pathway signaling regulator β-catenin, were on average up to five times more sensitive to TTK inhibitors than cell lines wild-type for CTNNB1. The association of CTNNB1-mutant status and increased cancer cell line sensitivity to TTK inhibition was confirmed with isogenic cell line pairs harboring either mutant or wild-type CTNNB1. Treatment of a xenograft model of a CTNNB1-mutant cell line with the TTK inhibitor NTRC 0066-0 resulted in complete inhibition of tumor growth. Mutations in CTNNB1 occur at relatively high frequency in endometrial cancer and hepatocellular carcinoma, which are known to express high TTK levels. We propose mutant CTNNB1 as a prognostic drug response biomarker, enabling the selection of patients most likely to respond to TTK inhibitor therapy in proof-of-concept clinical trials. Mol Cancer Ther; 16(11); 2609–17. ©2017 AACR.

Published

2023

7. Supplementary Figure S1 from Combined Cellular and Biochemical Profiling to Identify Predictive Drug Response Biomarkers for Kinase Inhibitors Approved for Clinical Use between 2013 and 2017

Author

Guido J.R. Zaman, Rogier C. Buijsman, Suzanne J.C. van Gerwen, Jos de Man, Masaaki Sawa, Yusuke Kawase, Nicole Willemsen-Seegers, Jelle Dylus, Martine B.W. Prinsen, Jeroen A.D.M. de Roos, Jeffrey J. Kooijman, and Joost C.M. Uitdehaag

Abstract

Workflow for filtering cell line genomic data

Published

2023

8. Supplementary Figure S1 from Cell Panel Profiling Reveals Conserved Therapeutic Clusters and Differentiates the Mechanism of Action of Different PI3K/mTOR, Aurora Kinase and EZH2 Inhibitors

Author

Guido J.R. Zaman, Rogier C. Buijsman, Jos de Man, Suzanne J.C. van Gerwen, Masaaki Sawa, Jeffrey Kooijman, Antoon M. van Doornmalen, Jelle Dylus, Judith R.F. de Vetter, Nicole Willemsen-Seegers, Martine B.W. Prinsen, Jeroen A.D.M. de Roos, and Joost C.M. Uitdehaag

Abstract

Additional reproducibility data

Published

2023

9. Figure S3 from TTK Inhibitors as a Targeted Therapy for CTNNB1 (β-catenin) Mutant Cancers

Author

Joost C.M. Uitdehaag, Rogier C. Buijsman, Jos de Man, Martine B.W. Prinsen, Marion A.A. Libouban, Jeroen A.D.M. de Roos, and Guido J.R. Zaman

Abstract

Beta-catenin pathway is activated in CTNNB1 mutant cell lines, and TTK inhibition has no direct regulatory effect on beta-catenin

Published

2023

10. Combined Cellular and Biochemical Profiling to Identify Predictive Drug Response Biomarkers for Kinase Inhibitors Approved for Clinical Use between 2013 and 2017

Author

Joost C.M. Uitdehaag, Rogier C. Buijsman, Guido J.R. Zaman, Masaaki Sawa, Jelle Dylus, Jeffrey J. Kooijman, Martine B.W. Prinsen, Suzanne J.C. van Gerwen, Yusuke Kawase, Nicole Willemsen-Seegers, Jeroen A.D.M. de Roos, and Jos de Man

Subjects

0301 basic medicine, Cancer Research, Small Molecule Libraries, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Piperidines, Cell Line, Tumor, Neoplasms, Humans, Point Mutation, Medicine, Protein Interaction Maps, Drug Approval, Protein Kinase Inhibitors, Cell Proliferation, Cobimetinib, Regulation of gene expression, Kinase, business.industry, Adenine, Point mutation, Drug Repositioning, Gene Expression Regulation, Neoplastic, Drug repositioning, Pyrimidines, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, ALK Gene Translocation, Ibrutinib, Cancer research, Pyrazoles, business, V600E

Abstract

Kinase inhibitors form the largest class of precision medicine. From 2013 to 2017, 17 have been approved, with 8 different mechanisms. We present a comprehensive profiling study of all 17 inhibitors on a biochemical assay panel of 280 kinases and proliferation assays of 108 cancer cell lines. Drug responses of the cell lines were related to the presence of frequently recurring point mutations, insertions, deletions, and amplifications in 15 well-known oncogenes and tumor-suppressor genes. In addition, drug responses were correlated with basal gene expression levels with a focus on 383 clinically actionable genes. Cell lines harboring actionable mutations defined in the FDA labels, such as mutant BRAF(V600E) for cobimetinib, or ALK gene translocation for ALK inhibitors, are generally 10 times more sensitive compared with wild-type cell lines. This sensitivity window is more narrow for markers that failed to meet endpoints in clinical trials, for instance CDKN2A loss for CDK4/6 inhibitors (2.7-fold) and KRAS mutation for cobimetinib (2.3-fold). Our data underscore the rationale of a number of recently opened clinical trials, such as ibrutinib in ERBB2- or ERBB4-expressing cancers. We propose and validate new response biomarkers, such as mutation in FBXW7 or SMAD4 for EGFR and HER2 inhibitors, ETV4 and ETV5 expression for MEK inhibitors, and JAK3 expression for ALK inhibitors. Potentially, these new markers could be combined to improve response rates. This comprehensive overview of biochemical and cellular selectivities of approved kinase inhibitor drugs provides a rich resource for drug repurposing, basket trial design, and basic cancer research.

Published

2019

11. Author response for 'Pharmacological validation of TDO as a target for Parkinson’s disease'

Author

Rogier C. Buijsman, Joeri Johannes Petrus De Wit, Freek van Cauter, Michaela Tutone, Youri Adolfs, Michelle Muller, R. Jeroen Pasterkamp, Joost C.M. Uitdehaag, Mitch Hartog, Diep Vu-Pham, Nicole Willemsen-Seegers, Guido J.R. Zaman, Aletta D. Kraneveld, Antoon M. van Doornmalen, Jan Gerard Sterrenburg, Jos de Man, Paula Perez-Pardo, and Yvonne Grobben

Subjects

Parkinson's disease, business.industry, medicine, medicine.disease, business, Neuroscience

Published

2020

12. Targeting Indoleamine 2,3-Dioxygenase in Cancer Models Using the Novel Small Molecule Inhibitor NTRC 3883-0

Author

Anne M. van Altena, Leon F.A.G. Massuger, Winfried R. Mulder, Diep Vu-Pham, Joeri de Wit, Freek van Cauter, Yvonne Grobben, Judith E. den Ouden, Jos de Man, Antoon M. van Doornmalen, Joost C.M. Uitdehaag, Nicole Willemsen-Seegers, Jan Gerard Sterrenburg, Rogier C. Buijsman, Guido J.R. Zaman, Michelle Muller, and Martine B.W. Prinsen

Subjects

lcsh:Immunologic diseases. Allergy, indoleamine 2,3-dioxygenase, T cell, medicine.medical_treatment, Cell, Immunology, Melanoma, Experimental, CD8-Positive T-Lymphocytes, Small Molecule Libraries, Mice, Immune system, IDO1 inhibitor, All institutes and research themes of the Radboud University Medical Center, Cancer immunotherapy, In vivo, Cell Line, Tumor, medicine, Immunology and Allergy, Animals, Humans, Indoleamine-Pyrrole 2,3,-Dioxygenase, Indoleamine 2,3-dioxygenase, Kynurenine, Original Research, Cell Proliferation, cancer immunotherapy, immunosuppression, Chemistry, Tryptophan, Cancer, medicine.disease, Women's cancers Radboud Institute for Health Sciences [Radboudumc 17], medicine.anatomical_structure, ovarian cancer, Cell culture, Cancer research, syngeneic mouse model, lcsh:RC581-607

Abstract

Indoleamine 2,3-dioxygenase (IDO1) is a key regulator of immune suppression by catalyzing the oxidation of L-tryptophan. IDO1 expression has been related to poor prognosis in several cancers and to resistance to checkpoint immunotherapies. We describe the characterization of a novel small molecule IDO1 inhibitor, NTRC 3883-0, in a panel of biochemical and cell-based assays, and various cancer models. NTRC 3883-0 released the inhibitory effect of IDO1 on CD8-positive T cell proliferation in co-cultures of IDO1-overexpressing cells with healthy donor lymphocytes, demonstrating its immune modulatory activity. In a syngeneic mouse model using IDO1-overexpressing B16F10 melanoma cells, NTRC 3883-0 effectively counteracted the IDO1-induced modulation of L-tryptophan and L-kynurenine levels, demonstrating its in vivo target modulation. Finally, we studied the expression and activity of IDO1 in primary cell cultures established from the malignant ascites of ovarian cancer patients. In these cultures, IDO1 expression was induced upon stimulation with IFNγ, and its activity could be inhibited by NTRC 3883-0. Based on these results, we propose the use of ascites cell-based functional assays for future patient stratification. Our results are discussed in light of the recent discontinuation of clinical trials of more advanced IDO1 inhibitors and the reconsideration of IDO1 as a valid drug target.

Published

2020

13. TTK Inhibitors as a Targeted Therapy forCTNNB1(β-catenin) Mutant Cancers

Author

Rogier C. Buijsman, Jeroen A.D.M. de Roos, Marion Libouban, Jos de Man, Guido J.R. Zaman, Martine B.W. Prinsen, and Joost C.M. Uitdehaag

Subjects

0301 basic medicine, Cancer Research, Mutation, Kinase, medicine.medical_treatment, Regulator, Wnt signaling pathway, Cancer, Biology, medicine.disease_cause, medicine.disease, Molecular biology, Targeted therapy, 03 medical and health sciences, Spindle checkpoint, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Catenin, medicine

Abstract

The spindle assembly checkpoint kinase TTK (Mps1) is a key regulator of chromosome segregation and is the subject of novel targeted therapy approaches by small-molecule inhibitors. Although the first TTK inhibitors have entered phase I dose escalating studies in combination with taxane chemotherapy, a patient stratification strategy is still missing. With the aim to identify a genomic biomarker to predict the response of tumor cells to TTK inhibitor therapy, we profiled a set of preclinical and clinical TTK inhibitors from different chemical series on a panel of 66 genetically characterized cell lines derived from different tumors (Oncolines). Cell lines harboring activating mutations in the CTNNB1 gene, encoding the Wnt pathway signaling regulator β-catenin, were on average up to five times more sensitive to TTK inhibitors than cell lines wild-type for CTNNB1. The association of CTNNB1-mutant status and increased cancer cell line sensitivity to TTK inhibition was confirmed with isogenic cell line pairs harboring either mutant or wild-type CTNNB1. Treatment of a xenograft model of a CTNNB1-mutant cell line with the TTK inhibitor NTRC 0066-0 resulted in complete inhibition of tumor growth. Mutations in CTNNB1 occur at relatively high frequency in endometrial cancer and hepatocellular carcinoma, which are known to express high TTK levels. We propose mutant CTNNB1 as a prognostic drug response biomarker, enabling the selection of patients most likely to respond to TTK inhibitor therapy in proof-of-concept clinical trials. Mol Cancer Ther; 16(11); 2609–17. ©2017 AACR.

Published

2017

14. Target Residence Time-Guided Optimization on TTK Kinase Results in Inhibitors with Potent Anti-Proliferative Activity

Author

Rogier C. Buijsman, Martine B.W. Prinsen, Jan Gerard Sterrenburg, Jos de Man, Joost C.M. Uitdehaag, Marion Libouban, Jeroen A.D.M. de Roos, Guido J.R. Zaman, Nicole Willemsen-Seegers, Judith R.F. de Vetter, and Joeri Johannes Petrus De Wit

Subjects

Models, Molecular, 0301 basic medicine, Protein Conformation, Allosteric regulation, Antineoplastic Agents, Cell Cycle Proteins, Plasma protein binding, Protein Serine-Threonine Kinases, Biology, Crystallography, X-Ray, 03 medical and health sciences, 0302 clinical medicine, Structural Biology, Cell Line, Tumor, Humans, Protein kinase A, Protein Kinase Inhibitors, Molecular Biology, Triple-negative breast cancer, Cell Proliferation, Cell growth, Kinase, Protein-Tyrosine Kinases, Kinetics, Spindle checkpoint, 030104 developmental biology, Biochemistry, 030220 oncology & carcinogenesis, Cancer research, Tyrosine kinase, Protein Binding

Abstract

The protein kinase threonine tyrosine kinase (TTK; also known as Mps1) is a critical component of the spindle assembly checkpoint and a promising drug target for the treatment of aggressive cancers, such as triple negative breast cancer. While the first TTK inhibitors have entered clinical trials, little is known about how the inhibition of TTK with small-molecule compounds affects cellular activity. We studied the selective TTK inhibitor NTRC 0066-0, which was developed in our own laboratory, together with 11 TTK inhibitors developed by other companies, including Mps-BAY2b, BAY 1161909, BAY 1217389 (Bayer), TC-Mps1-12 (Shionogi), and MPI-0479605 (Myrexis). Parallel testing shows that the cellular activity of these TTK inhibitors correlates with their binding affinity to TTK and, more strongly, with target residence time. TTK inhibitors are therefore an example where target residence time determines activity in in vitro cellular assays. X-ray structures and thermal stability experiments reveal that the most potent compounds induce a shift of the glycine-rich loop as a result of binding to the catalytic lysine at position 553. This "lysine trap" disrupts the catalytic machinery. Based on these insights, we developed TTK inhibitors, based on a (5,6-dihydro)pyrimido[4,5-e]indolizine scaffold, with longer target residence times, which further exploit an allosteric pocket surrounding Lys553. Their binding mode is new for kinase inhibitors and can be classified as hybrid Type I/Type III. These inhibitors have very potent anti-proliferative activity that rivals classic cytotoxic therapy. Our findings will open up new avenues for more applications for TTK inhibitors in cancer treatment.

Published

2017

15. Stable aneuploid tumors cells are more sensitive to TTK inhibition than chromosomally unstable cell lines

Author

Jeroen A.D.M. de Roos, Zuzana Storchova, René H. Medema, Jos de Man, Nicole Willemsen-Seegers, Marion Libouban, R.C. Buijsman, Bastiaan B J Tops, Joost C.M. Uitdehaag, Guido J.R. Zaman, Jules P.P. Meijerink, Jelle Dylus, and Sara Mainardi

Subjects

0301 basic medicine, kinase inhibitor, Cell Survival, T cell, TTK, Aneuploidy, Antineoplastic Agents, Cell Cycle Proteins, Protein Serine-Threonine Kinases, Biology, 03 medical and health sciences, chemistry.chemical_compound, Cell Line, Tumor, Chromosomal Instability, Neoplasms, Chromosome instability, medicine, Humans, Mps1, Protein Kinase Inhibitors, Mitosis, Cell Proliferation, Genetics, Cancer, Protein-Tyrosine Kinases, medicine.disease, 3. Good health, Spindle checkpoint, 030104 developmental biology, medicine.anatomical_structure, Oncology, chemistry, Cell culture, Cancer research, M Phase Cell Cycle Checkpoints, chromosome instability, Research Paper, Reversine

Abstract

// Marion A.A. Libouban 1, 2 , Jeroen A.D.M. de Roos 1 , Joost C.M. Uitdehaag 1 , Nicole Willemsen-Seegers 1 , Sara Mainardi 2 , Jelle Dylus 1 , Jos de Man 1 , Bastiaan Tops 3 , Jules P.P. Meijerink 4 , Zuzana Storchova 5 , Rogier C. Buijsman 1 , Rene H. Medema 2 , Guido J.R. Zaman 1 1 Netherlands Translational Research Center B.V., Oss, The Netherlands 2 Netherlands Cancer Institute, Amsterdam, The Netherlands 3 Department of Pathology, Radboud University Medical Center, Nijmegen, The Netherlands 4 Princess Maxima Center for Pediatric Oncology, Utrecht, The Netherlands 5 University of Kaiserslautern, Kaiserslautern, Germany Correspondence to: Guido J.R. Zaman, email: guido.zaman@ntrc.nl Keywords: TTK, Mps1, kinase inhibitor, chromosome instability, aneuploidy Received: November 16, 2016 Accepted: March 03, 2017 Published: March 15, 2017 ABSTRACT Inhibition of the spindle assembly checkpoint kinase TTK causes chromosome mis-segregation and tumor cell death. However, high levels of TTK correlate with chromosomal instability (CIN), which can lead to aneuploidy. We show that treatment of tumor cells with the selective small molecule TTK inhibitor NTRC 0066-0 overrides the mitotic checkpoint, irrespective of cell line sensitivity. In stable aneuploid cells NTRC 0066-0 induced acute CIN, whereas in cells with high levels of pre-existing CIN there was only a small additional fraction of cells mis-segregating their chromosomes. In proliferation assays stable aneuploid cells were more sensitive than cell lines with pre-existing CIN. Tetraploids are thought to be an intermediate between diploid and unstable aneuploid cells. TTK inhibitors had the same potency on post-tetraploid and parental diploid cells, which is remarkable because the post-tetraploids are more resistant to mitotic drugs. Finally, we confirm that the reference compound reversine is a TTK inhibitor and like NTRC 0066-0, inhibits the proliferation of patient-derived colorectal cancer organoids. In contrast, treatment with TTK inhibitor did not reduce the viability of non-proliferating T cell acute lymphoblastic leukemia cells samples. Consequently, TTK inhibitor therapy is expected to spare non-dividing cells, and may be used to target stable aneuploid tumors.

Published

2017

16. Cell Panel Profiling Reveals Conserved Therapeutic Clusters and Differentiates the Mechanism of Action of Different PI3K/mTOR, Aurora Kinase and EZH2 Inhibitors

Author

Jelle Dylus, Suzanne J.C. van Gerwen, Jeroen A.D.M. de Roos, Jeffrey J. Kooijman, Rogier C. Buijsman, Joost C.M. Uitdehaag, Jos de Man, Nicole Willemsen-Seegers, Judith R.F. de Vetter, Guido J.R. Zaman, Masaaki Sawa, Antoon M. van Doornmalen, and Martine B.W. Prinsen

Subjects

Proteomics, 0301 basic medicine, Cancer Research, DNA Copy Number Variations, Antineoplastic Agents, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, Aurora kinase, Aurora Kinases, Cell Line, Tumor, Cluster Analysis, Humans, Bruton's tyrosine kinase, Enhancer of Zeste Homolog 2 Protein, Protein Kinase Inhibitors, Protein kinase B, PI3K/AKT/mTOR pathway, Cell Proliferation, Phosphoinositide-3 Kinase Inhibitors, EGFR inhibitors, biology, Kinase, Cell growth, Gene Expression Profiling, TOR Serine-Threonine Kinases, Molecular biology, 030104 developmental biology, Oncology, Mutation, Cancer research, biology.protein, Signal transduction, Signal Transduction

Abstract

Cancer cell line panels are important tools to characterize the in vitro activity of new investigational drugs. Here, we present the inhibition profiles of 122 anticancer agents in proliferation assays with 44 or 66 genetically characterized cancer cell lines from diverse tumor tissues (Oncolines). The library includes 29 cytotoxics, 68 kinase inhibitors, and 11 epigenetic modulators. For 38 compounds this is the first comparative profiling in a cell line panel. By strictly maintaining optimized assay protocols, biological variation was kept to a minimum. Replicate profiles of 16 agents over three years show a high average Pearson correlation of 0.8 using IC50 values and 0.9 using GI50 values. Good correlations were observed with other panels. Curve fitting appears a large source of variation. Hierarchical clustering revealed 44 basic clusters, of which 26 contain compounds with common mechanisms of action, of which 9 were not reported before, including TTK, BET and two clusters of EZH2 inhibitors. To investigate unexpected clusterings, sets of BTK, Aurora and PI3K inhibitors were profiled in biochemical enzyme activity assays and surface plasmon resonance binding assays. The BTK inhibitor ibrutinib clusters with EGFR inhibitors, because it cross-reacts with EGFR. Aurora kinase inhibitors separate into two clusters, related to Aurora A or pan-Aurora selectivity. Similarly, 12 inhibitors in the PI3K/AKT/mTOR pathway separated into different clusters, reflecting biochemical selectivity (pan-PI3K, PI3Kβγδ-isoform selective or mTOR-selective). Of these, only allosteric mTOR inhibitors preferentially targeted PTEN-mutated cell lines. This shows that cell line profiling is an excellent tool for the unbiased classification of antiproliferative compounds. Mol Cancer Ther; 15(12); 3097–109. ©2016 AACR.

Published

2016

17. Abstract B060: Side-by-side comparison of small molecule IDO1 inhibitors in biochemical and cell-based assays and development of a IDO1-expressing mouse model to evaluate target modulation

Author

Rogier C. Buijsman, Diep Vu-Pham, Jos de Man, Joost C.M. Uitdehaag, Guido J.R. Zaman, Antoon M. van Doornmalen, Nicole Willemsen-Seegers, and Yvonne Grobben

Subjects

chemistry.chemical_classification, Cancer Research, Tumor microenvironment, Chemistry, Cell, HEK 293 cells, Molecular biology, Small molecule, Natural killer cell, medicine.anatomical_structure, Enzyme, Oncology, In vivo, Cell culture, medicine

Abstract

Introduction: Indoleamine 2,3-dioxygenase (IDO1) is a heme-containing oxidoreductase enzyme that converts L-tryptophan (Trp) into N’-formylkynurenine (NFK). IDO1 is broadly expressed by tumor cells as well as immune cells in the tumor microenvironment of many cancers, which is often correlated with poor prognosis. Depletion of Trp and increased L-kynurenine (Kyn) levels induce immune tolerance by suppression of effector T-cell and natural killer cell functions, and activation of regulatory T-cells and myeloid-derived suppressor cells. Four small molecule inhibitors are currently investigated in phase III (linrodostat/BMS-986205), phase II (epacadostat/INCB024360) or phase I (MK7162 and LY3381916) clinical trials. Linrodostat, epacadostat and LY3381916 are reported as being selective for IDO1 over TDO, while details on MK7162 have not yet been disclosed. The compounds inhibit IDO1 with different mechanisms, with epacadostat binding to the heme-group in the catalytic center of IDO1, while linrodostat and LY3381916 bind to apo-IDO1 and compete with heme for the active site [1-3]. Experimental procedures Clinical and reference IDO1 inhibitors were characterized in biochemical assays for IDO1 and tryptophan 2,3-dioxygenase (TDO), a structurally different enzyme, which also catalyzes the conversion of Trp to NFK. Furthermore, the compounds were profiled in a panel of functional cell-based assays, including human cancer cell lines and assays based on IDO1- or TDO2-overexpressing HEK293 cells. A IDO1-expressing subline of the mouse B16F10 melanoma cell line was generated and used to develop a syngeneic mouse model at Charles River Laboratories (USA) to determine target modulation in vivo [4]. Stable gene expression was confirmed by qPCR and target modulation was examined by measurement of Trp and Kyn levels using LC-MS/MS. Results: Linrodostat has sub-nanomolar cellular potency, despite the absence of any biochemical activity on the timescale of our assays, which is consistent with its reported heme-competing mechanism of inhibition [1]. Linrodostat also inhibits different Cytochrome P450 enzymes with micromolar activity. In our biochemical assays, epacadostat was not selective for IDO1 over TDO, whereas in the IDO1- and TDO2-overexpressing HEK293 cell lines it was 2000 times selective for IDO1. High level expression of IDO1 in B16F10 cells did not result in enhanced tumor growth after grafting in syngeneic mice, which contrasts published data with a similar model [4]. Nonetheless, we observed strong modulation of Trp and Kyn levels in plasma and in tumors of the IDO1-overexpressing mouse model, compared to non-tumor bearing mice. Treatment of the B16F10-IDO1 model with epacadostat did not result in a reduction of tumor growth, though epacadostat did induce clear changes in Trp and Kyn in both plasma and tumor tissue. Conclusion: Our comparative study of the potencies and selectivities of IDO1 inhibitors, as well as our model for measuring in vivo target modulation, helps to identify strengths and weaknesses of current IDO1 inhibitors, and supports the development of new inhibitors. [1] Nelp et al. (2018) Proc. Natl. Acad. Sci. U.S.A. 115, 3249-3254; [2] Yue et al. (2017) ACS Med. Chem. Lett. 8, 486-491; [3] Dorsey et al. (2018) Proceedings: AACR Annual Meeting 2018, Abstract nr. 5245; [4] Holmgaard et al. (2015) Cell Rep. 13, 412-424. Citation Format: Yvonne Grobben, Joost C.M. Uitdehaag, Antoon M. van Doornmalen, Nicole Willemsen-Seegers, Diep Vu-Pham, Jos de Man, Rogier C. Buijsman, Guido J.R. Zaman. Side-by-side comparison of small molecule IDO1 inhibitors in biochemical and cell-based assays and development of a IDO1-expressing mouse model to evaluate target modulation [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference on Molecular Targets and Cancer Therapeutics; 2019 Oct 26-30; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Ther 2019;18(12 Suppl):Abstract nr B060. doi:10.1158/1535-7163.TARG-19-B060

Published

2019

18. Abstract A044: A precision medicine platform to predict the clinical response to chemo- and immunotherapy for epithelial ovarian cancer

Author

Guido J.R. Zaman, Winfried R. Mulder, Antoon M. van Doornmalen, Jelle Dylus, Leon F.A.G. Massuger, Rogier C. Buijsman, Suzanne J.C. van Gerwen, Anne M. van Altena, Joost C.M. Uitdehaag, Diep Vu-Pham, and Judith E. den Ouden

Subjects

Neuroblastoma RAS viral oncogene homolog, Cancer Research, business.industry, medicine.medical_treatment, Cancer, Immunotherapy, Gene mutation, Debulking, medicine.disease, chemistry.chemical_compound, Immune system, Oncology, Paclitaxel, chemistry, medicine, Cancer research, business, Ovarian cancer

Abstract

Introduction: Epithelial ovarian cancer (EOC) is the most lethal gynecologic malignancy. First-line therapy in advanced EOC is surgery in combination with platinum-based chemotherapy and paclitaxel. 15-20% of patients do not respond and in 80% of advanced cases, the disease recurs within three years. PARP inhibitors synergize with platinum therapy and have been approved for platinum sensitive EOC. Clinical trials with immunotherapies, such as PD-1/PD-L1 blockade, have so far not been successful. Currently, the only approved companion diagnostic is BRCA gene mutations for PARP inhibitors. More diagnostic assays to predict the clinical response to chemo- or immunotherapies are needed. We have developed a biomarker discovery platform using ascites of ovarian cancer patients. Experimental procedures Ascites was gathered from patients by punction or during debulking surgery. Cells were collected by centrifugation and characterized by flow cytometry using specific antibodies. Genomic DNA was sequenced using Illumina cancer gene panels. Gene expression was analyzed by quantitative PCR (qPCR). Cellular activity of the tryptophan metabolizing enzymes IDO1 and TDO was measured with NFK Green [1]. Levels of L-tryptophan and its metabolite L-kynurenine in ascites fluid and blood were determined with LC-MS/MS. In vitro data were related to tumor histopathology and clinical response data. Results: Low passage cell samples from twenty patients were profiled for sensitivity to various cytotoxic agents and targeted anti-cancer therapies in cell proliferation assays. In parallel the mutation status of fifty cancer genes including BRCA1 and 2 was assessed by DNA sequencing. The expression of genes implicated in resistance to chemotherapy (CCNE1, ABCB1) or immunotherapy (PD-L1, IDO1, TDO) was determined with qPCR. The immune status of ascites was analyzed by measuring the relative proportion of different immune cell populations, i.e., cytotoxic and regulatory T cells, monocytes, dendritic and natural killer cells. The expression of the immune suppressive markers PD-L1, IDO1 and TDO was related to the immune cell composition of the ascites, kynurenine-tryptophan ratio, and clinical response data. A tumor cell sample derived from a patient with low grade serous ovarian cancer (LGSOC) was heterozygous for an oncogenic NRAS mutation and was much more sensitive to MEK inhibitors than other samples not harboring the mutation. The cells also expressed IDO1 and high levels of PD-L1 at the cell surface. Two other samples derived from high grade serous ovarian cancer (HGSOC) expressed high PD-L1 and one also IDO1. Several HGSOC samples expressed TDO. One HGSOC sample showed high expression of the ABCB1 gene, encoding the multidrug transporter P-glycoprotein. The sample was relatively resistant to paclitaxel, a known substrate of P-glycoprotein Conclusion: Our study shows that in vitro drug sensitivity assays with primary patient samples can be used to confirm or identify predictive drug response biomarkers. In an ongoing study, in which hundred patients with HGSOC will be included, the in vitro drug response of tumor cells from ascites to first-line cytotoxic anti-cancer agents will be determined and compared to the clinical response of patients bearing specific genomic biomarkers. [1] Seegers et al. (2014) J Biomol Screen 19, 1266-1272 Citation Format: Guido J.R. Zaman, Judith E. den Ouden, Jelle Dylus, Antoon M. van Doornmalen, Winfried R. Mulder, Diep Vu-Pham, Suzanne J.C. van Gerwen, Joost C.M. Uitdehaag, Rogier C. Buijsman, Leon F. Massuger, Anne M. van Altena. A precision medicine platform to predict the clinical response to chemo- and immunotherapy for epithelial ovarian cancer [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference on Molecular Targets and Cancer Therapeutics; 2019 Oct 26-30; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Ther 2019;18(12 Suppl):Abstract nr A044. doi:10.1158/1535-7163.TARG-19-A044

Published

2019

19. Abstract A141: Computational models of synergy contribute to efficient combination screening

Author

Jelle Dylus, Guido J.R. Zaman, Jeffrey J. Kooijman, Derek W. van Tilborg, Joost C.M. Uitdehaag, Suzanne J.C. van Gerwen, Rogier C. Buijsman, Martine B.W. Prinsen, Jos de Man, and Jeroen A.D.M. de Roos

Subjects

Drug, Cancer Research, Computational model, Computer science, media_common.quotation_subject, Cell panel, Cancer therapy, Computational biology, Gene mutation, Oncology, Cancer cell, Molecular targets, media_common, Combination drug

Abstract

Introduction: Combination drug treatment in cancer therapy aims to improve response rate and decrease the development of drug resistance. The discovery of novel drug combinations is constrained by the cost and effort of carrying out large unbiased screens and is hampered by poor translation towards the clinic. We investigate if computational models combined with screening can more efficiently reveal synergistic combinations and improve translation towards the clinic. The models are based on three different biological views of synergy. First, compounds that exploit similar vulnerabilities in cancer cells frequently show synergy in a particular genetic context (targeted synergy, model 1) [1,2]. Secondly, drugs with non-overlapping resistance mechanisms often yield clinically relevant drug combinations (model 2) [3]. Finally, drugs that mimic synthetic lethal interactions will often act synergistically (model 3) [4]. Experimental procedures Oncolines™ is a panel of 102 genetically characterized cell lines from diverse tumor origins, on which proliferation assays are run in parallel in nine-point dose-response curves. In this cell panel we profiled 162 different cancer therapeutics, including many standard of care, chemotherapeutic agents, epigenetic modulators, and approved and pre-clinical drugs such as CDK4/6, ALK and PI3K-inhibitors [5]. Cancer hotspot mutations and gene expression data were downloaded from the DepMap and CCLE databases. ANOVA and Pearson correlations were used to analyze the single agent response and genetic data in the statistical software R, to determine gene mutation (model 1) and resistance markers (model 2). For model 3, clinically relevant synthetic lethal pairs were combined with gene expression data [4]. The methods were used to predict results from published synergy screens, e.g. DREAM [6] and results from an independent experiment (NTRC SynergyScreen™) in which fixed concentrations of the poly-ADP ribose polymerase (PARP) inhibitor niraparib and the BET bromodomain inhibitor JQ1, were combined with nine-point dose-response curves of 150 anticancer agents. Synergies were quantified using curve-shift and CI-index. Results: Using a cancer cell line IC50 profile of a compound (such as Oncolines™), all three computational models of synergy prediction can be applied. Method 1 is successful in predicting combinations that augment a targeted effect, such as combining BRAF and MEK inhibitors in BRAF-mutant cancer [1]. Method 2 does not distinguish between additive or synergistic combinations but can identify clinically relevant combinations [3]. For method 3, a tool was developed that computationally assesses if drug pairs can pharmacologically mimic clinically validated synthetic lethal interactions [4]. This can predict DREAM data with a high AUC of 0.67 in a ROC curve. The tool successfully predicts synergy between niraparib and the SUMO inhibitor 2-D08, and niraparib and BCL2 inhibitors, which we observed in our screen. Conclusions: Computational tools for synergy have predictive value and can be useful to prioritize libraries for empirical combination screening. References: [1] Uitdehaag et al. (2015). PLoS ONE 10(5): e0125021. [2] Seashore-Ludlow et al. (2015) Cancer Discovery, 5: 1210-1223. [3] Palmer et al. (2017) Cell 171: 1678-1691. [4] Lee et al. (2018). Nature Communications 9: 2546. [5] Uitdehaag et al. (2016). Mol. Cancer Ther. 15: 3097-3109. [6] Menden et al. (2019) Nature Communications 10: 2674. Citation Format: Joost C.M. Uitdehaag, Martine B.W. Prinsen, Derek W. van Tilborg, Jeffrey J. Kooijman, Jelle Dylus, Jeroen A.D.M. de Roos, Suzanne J.C. van Gerwen, Jos de Man, Rogier C. Buijsman, Guido J.R. Zaman. Computational models of synergy contribute to efficient combination screening [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference on Molecular Targets and Cancer Therapeutics; 2019 Oct 26-30; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Ther 2019;18(12 Suppl):Abstract nr A141. doi:10.1158/1535-7163.TARG-19-A141

Published

2019

20. Abstract 2158: Combining cell panel profiling and synthetic lethality data to efficiently screen for synergistic combinations

Author

Joost C.M. Uitdehaag, Jeroen A.D.M. de Roos, Jeffrey J. Kooijman, Derek W. van Tilborg, Suzanne J.C. van Gerwen, Rogier C. Buijsman, Guido J.R. Zaman, Jelle Dylus, Jos de Man, and Martine B.W. Prinsen

Subjects

Cancer Research, Standard of care, Oncology, Computer science, Mechanism (biology), High-throughput screening, Cell panel, Cancer therapy, Synthetic lethality, Computational biology, Combination drug

Abstract

In cancer therapy, combination drug treatment aims to improve response rate and decrease the development of drug resistance. The discovery of new effective drug combinations is constrained by the cost and effort of carrying out large unbiased screens and by poor translation of results towards the clinic. Here we describe how focusing on the biological mechanisms underlying the activity of drug candidates may aid a priori selection of promising synergy candidates and help in translate synergistic combinations towards a clinical situation. We have previously shown [1] that curve shift analysis as developed by Straetemans et al. [2] is a better method than combination-matrix screening. Also a dose based score such as the isobologram or the CI-index more robustly assesses synergy than an effect-based score such as the Bliss-additivity [1]. On this basis, we developed a two-step synergy screening approach, called SynergyScreen™. By distinguishing separate synergy screening and synergy confirmation stages, this setup capitalizes on insights from high throughput screening to discover robust and reproducible pharmacologically synergistic pairs. To further improve the efficiency of synergy screening, we focused on pre-selecting compounds in our screening library according to their biological mechanism. We profiled a library of more than 160 anti-cancer agents in a cell panel of 102 cell lines from diverse tumor origins [3]. Agents were clustered according to response and so-called exemplars were collected into a focused library that represents the spectrum of biological mechanisms of current cancer therapy. This synergy screening library includes many standard of care chemotherapeutic agents, approved and pre-clinical kinase inhibitors, epigenetic modulators and compounds acting by other mechanisms. Finally, we harnassed recent insights into the biology of synergy to understand and predict synergistic pairs. A tool was developed that uses the response of a compound in a 102 cell line panel to pick potential synergistic partners from the database of preprofiled compounds. It does this by computationally assessing if pairs can pharmacologically mimick clinically validated synthetic lethal interactions [4]. We optimized prediction accuracy using the results of internal and external synergy screens. The tool was applied to specifically enrich test libraries and to predict synergies at clinically relevant doses, including the results of a SynergyScreen™ with the poly-ADP ribose polymerase (PARP) inhibitor niraparib and the BET bromodomain inhibitor JQ1. References [1] Uitdehaag et al. (2015). PLoS ONE 10(5): e0125021. [2] Straetemans et al. (2005). Biometrical J. 47, 299-308. [3] Uitdehaag et al. (2016). Mol. Cancer Ther. 15, 3097-3109. [4] Lee et al. (2018). Nature Communications 9, 2546. Citation Format: Joost C. Uitdehaag, Derek W. van Tilborg, Martine B.W. Prinsen, Jeffrey J. Kooijman, Jelle Dylus, Jeroen A.D.M. de Roos, Suzanne J.C. van Gerwen, Jos de Man, Rogier C. Buijsman, Guido J.R. Zaman. Combining cell panel profiling and synthetic lethality data to efficiently screen for synergistic combinations [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2019; 2019 Mar 29-Apr 3; Atlanta, GA. Philadelphia (PA): AACR; Cancer Res 2019;79(13 Suppl):Abstract nr 2158.

Published

2019

21. Identification of an evolutionary conserved structural loop that is required for the enzymatic and biological function of tryptophan 2,3-dioxygenase

Author

Ido P. Kema, Helen Michels, Joost C.M. Uitdehaag, Celine N. Martineau, Mandy Koopman, Renée I. Seinstra, R.C. Buijsman, Martijn van Faassen, Ellen A. A. Nollen, Guided Treatment in Optimal Selected Cancer Patients (GUTS), and Lifestyle Medicine (LM)

Subjects

MECHANISM, 0301 basic medicine, Aging, Kynurenine pathway, Amino Acid Motifs, Longevity, INHIBITION, ELEGANS, Sequence alignment, Plasma protein binding, Biology, Article, DISEASE, Evolution, Molecular, KYNURENINE PATHWAY, 03 medical and health sciences, 0302 clinical medicine, Animals, Humans, Amino Acid Sequence, Caenorhabditis elegans, Caenorhabditis elegans Proteins, Peptide sequence, chemistry.chemical_classification, Multidisciplinary, Tryptophan, biology.organism_classification, HEME, Tryptophan Oxygenase, Protein Structure, Tertiary, MODEL, 030104 developmental biology, Enzyme, Biochemistry, chemistry, Mutagenesis, DIOXYGENASES, CRISPR-Cas Systems, Sequence Alignment, Locomotion, 030217 neurology & neurosurgery, Function (biology), Protein Binding

Abstract

The enzyme TDO (tryptophan 2,3-dioxygenase; TDO-2 in Caenorhabditis elegans) is a potential therapeutic target to cancer but is also thought to regulate proteotoxic events seen in the progression of neurodegenerative diseases. To better understand its function and develop specific compounds that target TDO we need to understand the structure of this molecule. In C. elegans we compared multiple different CRISPR/Cas9-induced tdo-2 deletion mutants and identified a motif of three amino acids (PLD) that is required for the enzymatic conversion of tryptophan to N-formylkynurenine. Loss of TDO-2’s enzymatic activity in PDL deletion mutants was accompanied by an increase in motility during aging and a prolonged lifespan, which is in line with the previously observed phenotypes induced by a knockdown of the full enzyme. Comparison of sequence structures suggests that blocking this motif might interfere with haem binding, which is essential for the enzyme’s activity. The fact that these three residues are situated in an evolutionary conserved structural loop of the enzyme suggests that the findings can be translated to humans. The identification of this specific loop region in TDO-2–essential for its catalytic function–will aid in the design of novel inhibitors to treat diseases in which the TDO enzyme is overexpressed or hyperactive.

Published

2016

22. Compound Selectivity and Target Residence Time of Kinase Inhibitors Studied with Surface Plasmon Resonance

Author

Judith R.F. de Vetter, Rogier C. Buijsman, Martine B.W. Prinsen, Yusuke Kawase, Joost C.M. Uitdehaag, Nicole Willemsen-Seegers, Guido J.R. Zaman, Masaaki Sawa, and Jos de Man

Subjects

0301 basic medicine, Insecta, Stereochemistry, Aurora B kinase, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, Phosphatidylinositol 3-Kinases, Structural Biology, Bruton's tyrosine kinase, Animals, Humans, Surface plasmon resonance, Molecular Biology, IC50, Protein Kinase Inhibitors, Phosphoinositide-3 Kinase Inhibitors, biology, Kinase, Biological activity, Surface Plasmon Resonance, Duvelisib, Dissociation constant, ErbB Receptors, 030104 developmental biology, chemistry, biology.protein

Abstract

Target residence time (τ) has been suggested to be a better predictor of the biological activity of kinase inhibitors than inhibitory potency (IC50) in enzyme assays. Surface plasmon resonance binding assays for 46 human protein and lipid kinases were developed. The association and dissociation constants of 80 kinase inhibitor interactions were determined. τ and equilibrium affinity constants (KD) were calculated to determine kinetic selectivity. Comparison of τ and KD or IC50 values revealed a strikingly different view on the selectivity of several kinase inhibitors, including the multi-kinase inhibitor ponatinib, which was tested on 10 different kinases. In addition, known pan-Aurora inhibitors resided much longer on Aurora B than on Aurora A, despite having comparable affinity for Aurora A and B. Furthermore, the γ/δ-selective PI3K inhibitor duvelisib and the δ-selective drug idelalisib had similar 20-fold selectivity for δ- over γ-isoform but duvelisib resided much longer on both targets.

Published

2016

23. A guide to picking the most selective kinase inhibitor tool compounds for pharmacological validation of drug targets

Author

Joost C.M. Uitdehaag, Husam Alwan, Jos de Man, Guido J.R. Zaman, Folkert Verkaar, and R.C. Buijsman

Subjects

Pharmacology, ABL, Drug discovery, Kinase, Cyclin-dependent kinase, Druggability, biology.protein, Structure–activity relationship, Biology, PLK1, Proto-oncogene tyrosine-protein kinase Src

Abstract

To establish the druggability of a target, genetic validation needs to be supplemented with pharmacological validation. Pharmacological studies, especially in the kinase field, are hampered by the fact that many reference inhibitors are not fully selective for one target. Fortunately, the initial trickle of selective inhibitors released in the public domain has steadily swelled into a stream. However, rationally picking the most selective tool compound out of the increasing amounts of available inhibitors has become progressively difficult due to the lack of accurate quantitative descriptors of drug selectivity. A recently published approach, termed ‘selectivity entropy’, is an improved way of expressing selectivity as a single-value parameter and enables rank ordering of inhibitors. We provide a guide to select the best tool compounds for pharmacological validation experiments of candidate drug targets using selectivity entropy. In addition, we recommend which inhibitors to use for studying the biology of the 20 most investigated kinases that are clinically relevant: Abl (ABL1), AKT1, ALK, Aurora A/B, CDKs, MET, CSF1R (FMS), EGFR, FLT3, ERBB2 (HER2), IKBKB (IKK2), JAK2/3, JNK1/2/3 (MAPK8/9/10), MEK1/2, PLK1, PI3Ks, p38α (MAPK14), BRAF, SRC and VEGFR2 (KDR).

Published

2012

24. Abstract 1944: High-throughput fluorescence-based assay for screening of Arginase I inhibitors for cancer immunotherapy

Author

Rogier C. Buijsman, Werner W. Tabak, Johan Friesen, Yvonne Grobben, Jan J. M. van Groningen, Jos de Man, Martine B.W. Prinsen, Guido J.R. Zaman, Suzanne J.C. van Gerwen, Helma Rutjes, Nicole Willemsen-Seegers, and Joost C.M. Uitdehaag

Subjects

Cancer Research, Thermal shift assay, Chemistry, Ligand binding assay, medicine.medical_treatment, Drug design, Small molecule, Molecular biology, Receptor–ligand kinetics, Arginase, Oncology, Cancer immunotherapy, medicine, ARG1

Abstract

Arginase I (ArgI) is an important small molecule drug target in cancer immunotherapy. Arg1 converts L-arginine into L-ornithine and urea. Recruitment of ArgI-expressing myeloid-derived suppressor cells (MSDCs) at a tumor site results in the depletion of L-arginine, which causes reduced proliferation of T-cells and natural killer cells and inhibition of the antitumor immune response. In patient material, MSDC-induced T-cell suppression can be reverted by arginase inhibitors. ArgI inhibitors work synergistically with checkpoint inhibitor therapy in syngeneic mouse models. In order to find novel inhibitors for ArgI, we developed a set of tools to enable screening and hit validation. The first is an activity assay that enables the high-throughput screening (HTS) of compound libraries. Previously reported arginase assays are poorly compatible with HTS due to the requirement of multiple reactions steps, harsh assay conditions, or the use of low-turnover substrates other than L-arginine. We developed a novel ArgI activity assay, which has a homogenous format and requires only two addition steps before readout. The assay makes use of a fluorescence readout and has a high robustness (Z'-factor > 0.7). Progression of the assay can be followed in real time, allowing for kinetic experiments. To investigate the false positive hit rate, the assay was screened at the Pivot Park Screening Centre with a library consisting of 233 compounds with known interference in other assay formats. Using a simple background signal control, the number of false positives in this library was minimized to below 0.2%. The assay was subsequently used to accurately determine the dissociation constants and binding kinetics of the reference inhibitors ABH, NOHA and CB1158. In order to validate the binding of screening hits to ArgI, we developed a thermal shift assay. We observed a shift in the ArgI melting temperature of up to 3.8°C after addition of the most potent inhibitors. In addition, we developed a Surface Plasmon Resonance binding assay. This showed that ABH and CB1158 have long residence times on ArgI. To allow the development of novel inhibitors through rational drug design, we successfully crystallized human ArgI in a novel space group with higher symmetry (P63) compared to those previously reported (space group P3), and without the presence of hemihedral twinning. We determined a series of high resolution (< 1.7 Å) crystal structures at various pH values and with several ligands. These demonstrate that a series of peptide flips lies at the basis of the pH-dependent symmetry of ArgI and its unusually high pH optimum of 9.0 to 9.5. Finally, to assess the cellular activity of ArgI inhibitors, we examined 102 cancer cell lines for ArgI activity and correlated the results to public gene expression profiles. The novel assay portfolio will help to deliver a new generation of ArgI inhibitors. Citation Format: Yvonne Grobben, Joost C. Uitdehaag, Nicole Willemsen-Seegers, Werner W. Tabak, Martine B. Prinsen, Suzanne J. van Gerwen, Jan van Groningen, Johan Friesen, Helma Rutjes, Jos de Man, Rogier C. Buijsman, Guido J. Zaman. High-throughput fluorescence-based assay for screening of Arginase I inhibitors for cancer immunotherapy [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 1944.

Published

2018

25. Design and optimization of a series of novel 2-cyano-pyrimidines as cathepsin K inhibitors

Author

Eric Nicolai, Clive Long, Ann Mitchell, Maureen Dempster, William Hamilton, Jennifer Kerr, Cecile Dorleans, Iain Martin, Paul Scullion, Hortense Deronzier, John Bruin, Emma Hamilton, Zoran Rankovic, Andre Fouquet, John Robinson, John Waller, Laurent Saniere, Mark Baugh, Fiona Andrews, Jiaqiang Cai, Joost C.M. Uitdehaag, Wilson Caulfield, Dominique Potin, Ashvin Mistry, François Chevallier, Paul Westwood, Emma Kinghorn, George McGarry, Iain Cumming, Mario van Zeeland, and X. Fradera

Subjects

Stereochemistry, Cathepsin K, Clinical Biochemistry, Administration, Oral, Pharmaceutical Science, Cysteine Proteinase Inhibitors, Crystallography, X-Ray, Biochemistry, Cathepsin A, Cell Line, Cathepsin C, Rats, Sprague-Dawley, Structure-Activity Relationship, Cathepsin O, Drug Discovery, Hydrolase, Animals, Humans, Structure–activity relationship, Molecular Biology, Binding Sites, Chemistry, Organic Chemistry, High-Throughput Screening Assays, Rats, Bioavailability, Pyrimidines, Drug Design, Molecular Medicine

Abstract

Morphing structural features of HTS-derived chemotypes led to the discovery of novel 2-cyano-pyrimidine inhibitors of cathepsin K with good pharmacokinetic profiles, for example, compound 20 showed high catK potency (IC(50)=4nM), >580-fold selectivity over catL and catB, and oral bioavailability in the rat of 52%.

Published

2010

26. The dependency game: Multiperson reciprocal sharing leads to stable cooperation which can evolve into group formation

Author

Joost C.M. Uitdehaag

Subjects

Statistics and Probability, Competitive Behavior, Computer science, media_common.quotation_subject, Population, Models, Psychological, Choice Behavior, General Biochemistry, Genetics and Molecular Biology, Microeconomics, Tit for tat, Game Theory, Memory, Humans, Simultaneous game, Cooperative Behavior, education, media_common, education.field_of_study, General Immunology and Microbiology, Applied Mathematics, General Medicine, Prisoner's dilemma, Group Processes, Action (philosophy), Modeling and Simulation, Repeated game, General Agricultural and Biological Sciences, Reciprocal, Reputation

Abstract

In the standard model for reciprocal collaboration, the repeated prisoner's dilemma (PD), it has proved difficult to establish collaboration in larger groups, necessitating the introduction of additional mechanisms such as reputation or assortedness. The problem is corroborated because current multiperson PDs model simultaneous player action, known as a common goods situation, whereas multiperson collaboration could be easier to obtain in a PD with alternate player action, a private goods situation. Here we present such a game, called a dependency game, and show that stable collaboration can be obtained in a 255 player simulation if only players are allowed to remember three previous benefactors, so they can play advanced tit-for-tat. Furthermore, we show that such a freely collaborating population is threatened by assorted strategies, which define groups that parasitize on independent tit-for-tat players. By excluding others, these groups engage in indirect reciprocal behaviour. Our model therefore combines many hitherto separate collaboration-enhancing concepts into one game, and suggests that group formation and collaboration are two separate social phenomena.

Published

2009

27. MEK and PI3K-AKT inhibitors synergistically block activated IL7 receptor signaling in T-cell acute lymphoblastic leukemia

Author

Kirsten Canté-Barrett, J. van der Zwet, Rob Pieters, Willem K. Smits, G.J.R. Zaman, R.C. Buijsman, Joost C.M. Uitdehaag, Jessica Buijs-Gladdines, Jules P.P. Meijerink, J.A.P. Spijkers-Hagelstein, and Pediatrics

Subjects

0301 basic medicine, Cancer Research, T cell, Biology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Transfection, 03 medical and health sciences, Mice, medicine, Tumor Cells, Cultured, Cytotoxic T cell, PTEN, Animals, Humans, Interleukin-7 receptor, Protein kinase B, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Cell Proliferation, Phosphoinositide-3 Kinase Inhibitors, Mitogen-Activated Protein Kinase Kinases, Receptors, Interleukin-7, Hematology, medicine.disease, Molecular biology, Leukemia, 030104 developmental biology, medicine.anatomical_structure, Oncology, biology.protein, Cancer research, Original Article, Signal transduction, Proto-Oncogene Proteins c-akt, Signal Transduction

Abstract

We identified mutations in the IL7Ra gene or in genes encoding the downstream signaling molecules JAK1, JAK3, STAT5B, N-RAS, K-RAS, NF1, AKT and PTEN in 49% of patients with pediatric T-cell acute lymphoblastic leukemia (T-ALL). Strikingly, these mutations (except RAS/NF1) were mutually exclusive, suggesting that they each cause the aberrant activation of a common downstream target. Expressing these mutant signaling molecules-but not their wild-type counterparts-rendered Ba/F3 cells independent of IL3 by activating the RAS-MEK-ERK and PI3K-AKT pathways. Interestingly, cells expressing either IL7Ra or JAK mutants are sensitive to JAK inhibitors, but respond less robustly to inhibitors of the downstream RAS-MEK-ERK and PI3K-AKT-mTOR pathways, indicating that inhibiting only one downstream pathway is not sufficient. Here, we show that inhibiting both the MEK and PI3K-AKT pathways synergistically prevents the proliferation of BaF3 cells expressing mutant IL7Ra, JAK and RAS. Furthermore, combined inhibition of MEK and PI3K/AKT was cytotoxic to samples obtained from 6 out of 11 primary T-ALL patients, including 1 patient who had no mutations in the IL7R signaling pathway. Taken together, these results suggest that the potent cytotoxic effects of inhibiting both MEK and PI3K/AKT should be investigated further as a therapeutic option using leukemia xenograft models.

Published

2016

28. Structural modeling of JAK1 mutations in T-cell acute lymphoblastic leukemia reveals a second contact site between pseudokinase and kinase domains

Author

Joost C.M. Uitdehaag, Jules P.P. Meijerink, Kirsten Canté-Barrett, and Pediatrics

Subjects

0301 basic medicine, Janus kinase 1, Kinase, Lymphoblastic Leukemia, T cell, Hematology, Janus Kinase 1, Review Article, Biology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Activating mutation, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Tyrosine kinase 2, Mutation, Cancer research, medicine, Humans, Janus kinase, Cytokine receptor

Abstract

Constitutive JAK-STAT pathway activation occurs in most myeloproliferative neoplasms as well as in a significant proportion of other hematologic malignancies, and is frequently a marker of poor prognosis. The underlying molecular alterations are heterogeneous as they include activating mutations in distinct components (cytokine receptor, JAK, STAT), overexpression (cytokine receptor, JAK) or rare JAK2 fusion proteins. In some cases, concomitant loss of negative regulators contributes to pathogenesis by further boosting the activation of the cascade. Exploiting the signaling bottleneck provided by the limited number of JAK kinases is an attractive therapeutic strategy for hematologic neoplasms driven by constitutive JAK-STAT pathway activation. However, given the conserved nature of the kinase domain among family members and the interrelated roles of JAK kinases in many physiological processes, including hematopoiesis and immunity, broad usage of JAK inhibitors in hematology is challenged by their narrow therapeutic window. Novel therapies are, therefore, needed. The development of more selective inhibitors is a questionable strategy as such inhibitors might abrogate the beneficial contribution of alleviating the cancer-related pro-inflammatory microenvironment and raise selective pressure to a threshold that allows the emergence of malignant subclones harboring drug-resistant mutations. In contrast, synergistic combinations of JAK inhibitors with drugs targeting cascades that work in concert with JAK-STAT pathway appear to be promising therapeutic alternatives to JAK inhibitors as monotherapies.

Published

2016

29. Localization of the Serine Protease-binding Sites in the Collagen-like Domain of Mannose-binding Protein

Author

Ce-Belle Chen, Jonathan M. Shaw, Russell Wallis, Joost C.M. Uitdehaag, Kurt Drickamer, and Dawn Torgersen

Subjects

Serine protease, Proteases, Protease binding, Mutant, Cell Biology, Biology, Biochemistry, Serine, Protein structure, biology.protein, Binding site, Molecular Biology, Peptide sequence

Abstract

Mutations in the collagen-like domain of serum mannose-binding protein (MBP) interfere with the ability of the protein to initiate complement fixation through the MBP-associated serine proteases (MASPs). The resulting deficiency in the innate immune response leads to susceptibility to infections. Studies have been undertaken to define the region of MBP that interacts with MASPs and to determine how the naturally occurring mutations affect this interaction. Truncated and modified MBPs and synthetic peptides that represent segments of the collagen-like domain of MBP have been used to demonstrate that MASPs bind on the C-terminal side of the hinge region formed by an interruption in the Gly-X-Y repeat pattern of the collagen-like domain. The binding sites for MASP-2 and for MASP-1 and -3 overlap but are not identical. The two most common naturally occurring mutations in MBP result in substitution of acidic amino acids for glycine residues in Gly-X-Y triplets on the N-terminal side of the hinge. Circular dichroism analysis and differential scanning calorimetry demonstrate that the triple helical structure of the collagen-like domain is largely intact in the mutant proteins, but it is more easily unfolded than in wild-type MBP. Thus, the effect of the mutations is to destabilize the collagen-like domain, indirectly disrupting the binding sites for MASPs. In addition, at least one of the mutations has a further effect on the ability of MBP to activate MASPs.

Published

2004

30. Abstract B155: Combining cell panel screening with analysis of gene expression levels reveals features of drug response and resistance

Author

Rogier C. Buijsman, Guido J.R. Zaman, Joost C.M. Uitdehaag, Jeroen A.D.M. de Roos, Suzanne J.C. van Gerwen, Martine B.W. Prinsen, Jeffrey J. Kooijman, and Jelle Dylus

Subjects

Cancer Research, biology, Drug discovery, Computational biology, Nutlin, Genomic Biomarker, chemistry.chemical_compound, Aurora kinase, Oncology, chemistry, ABCC3, Gene expression, biology.protein, Bruton's tyrosine kinase, Gene

Abstract

Screening of new drugs on large cell panels is an important tool to study the biologic mechanism of drug response. From a combination of parallel in vitro tests and bio-informatics analysis, important conclusions can be drawn, for instance about drug selectivity in a cellular context, about resistance mechanisms, and about the patient population in which a drug is effective. This makes cell panel screening indispensable in modern drug discovery. We have set up a platform called Oncolines™ that comprises 102 cell lines from diverse tumor tissues. All cell lines are screened in parallel in high-throughput proliferation assays based on ATP-lite™. Compounds are tested with 9 point dose-response curves in duplicate. Curves are visually inspected. In the past, we have shown that this workflow leads to highly reproducible IC50s, which are necessary for genomic biomarker discovery [1]. For instance, the IC50s have been coupled to curated databases of somatic mutations and copy numbers (1). However, these changes only reflect a small percentage of oncogenic transformations. A more comprehensive view of oncogenic signaling inside a cell can be obtained from mRNA expression levels (2). Here, we describe a workflow to investigate drug response in the 102 cell line Oncolines™ panel based on basal gene expression levels. Correlations between gene expression levels and the log IC50s were calculated for more than 18,000 genes. To reduce the number of false-positive correlations, we considered only genes with a known biologic role in cancer or that were clinically actionable. Secondly, we filtered out genes that correlated indiscriminately with drug responses, by correcting for the average correlations seen in our profiling database of more than 150 inhibitors. This filtered gene list was structured graphically by combining it with information on protein-protein interactions (using the StringDB) or information on which genes are part of the same pathways (a method called Gene Set Analysis). Our method reveals that gene overexpression correlates with drug responses for a number of targets. For instance, EGFR, IGFR, or ALK kinase inhibitors have more potent effects in cell lines that overexpress EGFR, IGFR, or ALK, respectively, and the MDM2 antagonist nutlin is more active in MDM2-overexpressing cell lines. This is irrespective of the genomic alterations driving overexpression of these genes. The distinct response profiles of the spectrum-selective BTK/EGFR/ERBB2 inhibitor ibrutinib and the more selective BTK inhibitor alcalabrutinib could be distinguished as well. Finally, the analysis shows mechanisms of drug resistance. For instance, the response of vincristine strongly correlates to cellular ABCB1 expression, the P-glycoprotein/MDR1 drug transporter, but also to ABCC3, another ABC transporter. Combining basal gene expression levels with cell panel data therefore allows discovery of novel mechanisms of drug response and resistance. References: 1. Uitdehaag et al. Cell panel profiling reveals conserved therapeutic clusters and differentiates the mechanism of action of different PI3K/mTOR, Aurora kinase and EZH2 inhibitors. Mol Cancer Therap 2016;15:3097-3109. 2. Rees et al. Correlating chemical sensitivity and basal gene expression reveals mechanism of action. Nature Chem Biol 2016;12:109-16. Citation Format: Joost C.M. Uitdehaag, Jeffrey Kooijman, Jeroen A.D.M. de Roos, Martine B.W. Prinsen, Jelle Dylus, Suzanne J.C. van Gerwen, Rogier C. Buijsman, Guido J.R. Zaman. Combining cell panel screening with analysis of gene expression levels reveals features of drug response and resistance [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference: Molecular Targets and Cancer Therapeutics; 2017 Oct 26-30; Philadelphia, PA. Philadelphia (PA): AACR; Mol Cancer Ther 2018;17(1 Suppl):Abstract nr B155.

Published

2018

31. Abstract B065: TTK inhibitors as a targeted therapy for β-catenin mutant cancers

Author

Jeroen A.D.M. de Roos, Joost C.M. Uitdehaag, Martine B.W. Prinsen, Marion Libouban, Guido J.R. Zaman, Jos de Man, and Rogier C. Buijsman

Subjects

Cancer Research, Kinase, Melanoma, medicine.medical_treatment, Wnt signaling pathway, Cancer, Biology, medicine.disease, Targeted therapy, Oncology, Catenin, Cancer cell, medicine, Cancer research, Kinase activity

Abstract

The dual-specificity protein kinase TTK, commonly referred to as Mps1, is a component of the spindle assembly checkpoint, a surveillance mechanism that ensures the fidelity of chromosome segregation. Inhibition of TTK kinase activity with small molecule kinase inhibitors leads to chromosome segregation errors by allowing mitotic exit in the presence of unattached kinetochores (1). After several rounds of cell division, the accumulation of chromosome segregation errors results in cancer cell death by apoptosis (2). Several TTK inhibitors have been shown to reduce the growth of xenografts of human cancer cell lines from diverse tumor tissue origin in mice. In an immunocompetent mouse model of triple-negative breast cancer (TNBC), TTK inhibitors increased the efficacy of taxane chemotherapy (1). While the first TTK inhibitors have entered phase 1 dose escalating studies in combination with taxane chemotherapy, a patient stratification strategy is still missing. To enable the selection of patients most likely to respond to TTK inhibitor therapy, we profiled a set of ten preclinical and clinical inhibitors (3) on a panel of 66 genetically characterized cancer cell lines derived from different tumor tissues (Oncolines) (4). Drug sensitivity was related to the mutation status of 114 cancer genes in an unbiased way. Cell lines harboring activating mutations in the CTNNB1 gene, encoding the Wnt pathway signaling regulator β-catenin, were on average up to five times more sensitive to TTK inhibitors than cell lines wild-type for CTNNB1. The association of CTNNB1 mutant status and increased cancer cell line sensitivity to TTK inhibition was confirmed with isogenic cell line pairs harboring either mutant or wild-type CTNNB1. Treatment of a xenograft model of a CTNNB1 mutant cell line with the TTK inhibitor NTRC 0066-0 resulted in complete inhibition of tumor growth. Mutations in CTNNB1 occur at relatively high frequency in endometrial cancer and hepatocellular carcinoma, which are known to express high TTK levels (5). Interestingly, β-catenin signaling has also been implicated in intrinsic resistance against immunotherapy in melanoma by regulation of T cell infiltration (6). We propose mutant CTNNB1 as a prognostic drug response biomarker, enabling the selection of patients most likely to respond to TTK inhibitor therapy in proof-of-concept clinical trials. References: 1. Maia et al. Ann Oncol 2015;26:2180-92; 2. Libouban et al. Oncotarget 2017;8:38309-25; 3. Uitdehaag et al. J Mol Biol 2017;429:2211-30; 4. Uitdehaag et al. Mol Cancer Ther 2016;15:3097-109; 5. Liu et al. Oncotarget 2015;6:34309-20; 6. Spranger et al. Nature 2015;523:231-5. Citation Format: Guido Zaman, Jeroen de Roos, Marion Libouban, Martine Prinsen, Jos de Man, Rogier Buijsman, Joost Uitdehaag. TTK inhibitors as a targeted therapy for β-catenin mutant cancers [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference: Molecular Targets and Cancer Therapeutics; 2017 Oct 26-30; Philadelphia, PA. Philadelphia (PA): AACR; Mol Cancer Ther 2018;17(1 Suppl):Abstract nr B065.

Published

2018

32. Selective Targeting of CTNNB1-, KRAS- or MYC-Driven Cell Growth by Combinations of Existing Drugs

Author

Rogier C. Buijsman, Martine B.W. Prinsen, Jeroen A.D.M. de Roos, Guido J.R. Zaman, Jill A. P. Spijkers-Hagelstein, Joost C.M. Uitdehaag, Jos de Man, Antoon M. van Doornmalen, and Judith R.F. de Vetter

Subjects

Proto-Oncogene Proteins B-raf, Indazoles, Indoles, Pyridones, Aurora inhibitor, lcsh:Medicine, Pyrimidinones, Biology, Pharmacology, Proto-Oncogene Proteins c-myc, Proto-Oncogene Proteins p21(ras), Cell Line, Tumor, Antineoplastic Combined Chemotherapy Protocols, Oximes, medicine, Humans, Molecular Targeted Therapy, Vemurafenib, lcsh:Science, Melanoma, Oxazoles, beta Catenin, Cell Proliferation, Trametinib, Aza Compounds, Sulfonamides, Multidisciplinary, MEK inhibitor, lcsh:R, Imidazoles, Correction, Dabrafenib, Triazoles, Mutation, Cancer cell, Neratinib, Quinolines, Cancer research, Benzimidazoles, lcsh:Q, Research Article, Combination drug, medicine.drug

Abstract

The aim of combination drug treatment in cancer therapy is to improve response rate and to decrease the probability of the development of drug resistance. Preferably, drug combinations are synergistic rather than additive, and, ideally, drug combinations work synergistically only in cancer cells and not in non-malignant cells. We have developed a workflow to identify such targeted synergies, and applied this approach to selectively inhibit the proliferation of cell lines with mutations in genes that are difficult to modulate with small molecules. The approach is based on curve shift analysis, which we demonstrate is a more robust method of determining synergy than combination matrix screening with Bliss-scoring. We show that the MEK inhibitor trametinib is more synergistic in combination with the BRAF inhibitor dabrafenib than with vemurafenib, another BRAF inhibitor. In addition, we show that the combination of MEK and BRAF inhibitors is synergistic in BRAF-mutant melanoma cells, and additive or antagonistic in, respectively, BRAF-wild type melanoma cells and non-malignant fibroblasts. This combination exemplifies that synergistic action of drugs can depend on cancer genotype. Next, we used curve shift analysis to identify new drug combinations that specifically inhibit cancer cell proliferation driven by difficult-to-drug cancer genes. Combination studies were performed with compounds that as single agents showed preference for inhibition of cancer cells with mutations in either the CTNNB1 gene (coding for β-catenin), KRAS, or cancer cells expressing increased copy numbers of MYC. We demonstrate that the Wnt-pathway inhibitor ICG-001 and trametinib acted synergistically in Wnt-pathway-mutant cell lines. The ERBB2 inhibitor TAK-165 was synergistic with trametinib in KRAS-mutant cell lines. The EGFR/ERBB2 inhibitor neratinib acted synergistically with the spindle poison docetaxel and with the Aurora kinase inhibitor GSK-1070916 in cell lines with MYC amplification. Our approach can therefore efficiently discover novel drug combinations that selectively target cancer genes.

Published

2015

33. Abstract 4185: NTRC 1501-0, a TTK kinase inhibitor selected for its long target residence time, completely inhibits tumor growth in the MDA-MB-231 xenograft model for triple-negative breast cancer

Author

Rogier C. Buijsman, Jeroen A.D.M. de Roos, Jos de Man, Marion Libouban, Nicole Willemsen-Seegers, Joost C.M. Uitdehaag, Martine B.W. Prinsen, Joeri Johannes Petrus De Wit, Guido J.R. Zaman, and Jan Gerard Sterrenburg

Subjects

Cancer Research, Kinase, Cell cycle, PLK1, chemistry.chemical_compound, Oncology, Paclitaxel, chemistry, Biochemistry, Protein kinase domain, Cancer research, Protein kinase A, Mitotic catastrophe, Mitosis

Abstract

The protein kinase TTK is a critical component of the spindle assembly checkpoint (SAC), which regulates the proper attachment of sister chromatids during mitosis. TTK is essential for normal progression of the cell cycle and is upregulated in various aggressive cancers such as triple negative breast cancer (TNBC). Inhibition of TTK leads to an overriding of the SAC, premature progression of the cell cycle and mitotic catastrophe. TTK inhibition therefore contrasts with e.g. Aurora and PLK1 inhibition, which block the cell cycle [1]. Various studies have shown the clinical utility of TTK inhibition, particularly in combination therapy with paclitaxel [1,2]. In vivo, TTK inhibitor monotherapy has shown partial tumor growth inhibition without weight loss [1,2]. We have developed a novel class of TTK inhibitors based on a pyrimido-indolizine scaffold. These bind selectively and with high affinity to the ATP pocket of TTK and potently inhibit the proliferation of a variety of cell lines [1]. Previously we published a representative of this class, NTRC 0066-0, which has an IC50 of 0.6 nM in a biochemical assay for TTK activity and which is more than 200 times selective over a panel of 276 kinases [1]. NTRC 0066-0 has an average IC50 of 98 nM in proliferation assays in 66 different cell lines (Oncolines™ panel) [3]. To further improve the potency of the pyrimido-indolizine series, we determined the X-ray structures of a dozen of class representatives in complex with TTK. The results were compared to 3D complexes of other chemical scaffolds such as BAY-1161909, Mps-Bay2b, MPI-0479605, NMS-P715 and Mps1-IN1. The pyrimido-indolizine series uses an aromatic moiety to trap the catalytic lysine in the active site, enforcing a catalytically incompetent conformation of TTK. Thermal melting and surface plasmon resonance experiments demonstrate that this leads to a strong stabilization of the kinase domain and a slow dissociation rate for the compounds, which is one of the key determinants for potent cellular activity. We took advantage of these structure-activity relationships to develop analogs of NTRC 0066-0 with increased residence time and cellular potency. One such analog, NTRC 1501-0, inhibits the proliferation of 66 cancer cell lines with an average IC50 of 18 nM, while retaining selectivity over the kinome. It has good pharmacokinetic properties and shows no cross-reactivity with drug safety targets in vitro. In a xenograft model of the human TNBC cell line MDA-MB-231, it completely inhibited tumor growth at a low oral dose, without effect on body weight, indicating good tolerability. These data show, for the first time, that TTK inhibition as monotherapy can achieve complete inhibition of tumor growth. [1] Maia et al. (2015) Annals of Oncology 26, 2180-2192; [2] Wengner et al (2016) Mol. Canc. Therap. 15, 583-592; [3] Uitdehaag et al. (2016) Mol. Canc. Therap., in the press. Citation Format: Joost C. Uitdehaag, Jos de Man, Marion Libouban, Nicole Willemsen-Seegers, Jan Gerard Sterrenburg, Joeri J. de Wit, Jeroen A.D de Roos, Martine B. Prinsen, Rogier C. Buijsman, Guido J. Zaman. NTRC 1501-0, a TTK kinase inhibitor selected for its long target residence time, completely inhibits tumor growth in the MDA-MB-231 xenograft model for triple-negative breast cancer [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 4185. doi:10.1158/1538-7445.AM2017-4185

Published

2017

34. High-throughput fluorescence-based screening assays for tryptophan-catabolizing enzymes

Author

Rogier C. Buijsman, Antoon M. van Doornmalen, Nicole Wilhelmina Cornelia Seegers, Joost C.M. Uitdehaag, Jos de Man, and Guido J.R. Zaman

Subjects

High-throughput screening, medicine.medical_treatment, Drug Evaluation, Preclinical, Chemical probe, Biology, Biochemistry, Catalysis, Analytical Chemistry, Cell Line, Small Molecule Libraries, Inhibitory Concentration 50, Cancer immunotherapy, medicine, Humans, Indoleamine-Pyrrole 2,3,-Dioxygenase, Enzyme Inhibitors, Indoleamine 2,3-dioxygenase, Enzyme Assays, Fluorescent Dyes, chemistry.chemical_classification, Excitation wavelength, Tryptophan, Fluorescence, Tryptophan Oxygenase, High-Throughput Screening Assays, Enzyme Activation, Enzyme, chemistry, Molecular Medicine, Biotechnology

Abstract

Indoleamine 2,3-dioxygenase (IDO1) and tryptophan 2,3-dioxygenase (TDO) are two structurally different enzymes that have a different tissue distribution and physiological roles, but both catalyze the conversion of tryptophan to N-formylkynurenine (NFK). IDO1 has been clinically validated as a small-molecule drug target for cancer, while preclinical studies indicate that TDO may be a target for cancer immunotherapy and neurodegenerative disease. We have developed a high-throughput screening assay for IDO1 and TDO based on a novel chemical probe, NFK Green, that reacts specifically with NFK to form a green fluorescent molecule with an excitation wavelength of 400 nm and an emission wavelength of 510 nm. We provide the first side-by-side comparison of a number of published inhibitors of IDO1 and TDO and reveal that the preclinical IDO1 inhibitor Compound 5l shows significant cross-reactivity with TDO, while the relative selectivity of other published inhibitors was confirmed. The suitability for high-throughput screening of the assays was demonstrated by screening a library of 87,000 chemical substances in 384- or 1536-well format. Finally, we demonstrate that the assay can also be used to measure the capacity of cells to metabolize tryptophan and to measure the cellular potency of IDO1 and TDO inhibitors.

Published

2014

35. The role of arginine 47 in the cyclization and coupling reactions of cyclodextrin glycosyltransferase from Bacillus circulans strain 251 - Implications for product inhibition and product specificity

Author

Joost C.M. Uitdehaag, Bauke W. Dijkstra, Bart A. van der Veen, Lubbert Dijkhuizen, and X-ray Crystallography

Subjects

Stereochemistry, 1.8-ANGSTROM RESOLUTION, ANGSTROM RESOLUTION, Bacillus, Cyclodextrin glycosyltransferase, CYCLOMALTODEXTRIN GLUCANOTRANSFERASE, Arginine, Biochemistry, X-RAY STRUCTURE, Substrate Specificity, BETA-CYCLODEXTRIN, THERMOANAEROBACTERIUM THERMOSULFURIGENES EM1, cyclodextrin glycosyltransferase, NUCLEOTIDE-SEQUENCE, Glycosyltransferase, Enzyme Stability, polycyclic compounds, Binding site, chemistry.chemical_classification, STARCH-DIGESTING AMYLASE, Binding Sites, cyclodextrins, MOLECULAR-CLONING, Cyclodextrin, biology, Chemistry, product specificity, Oligosaccharide, carbohydrates (lipids), Amino Acid Substitution, Product inhibition, Glucosyltransferases, ESCHERICHIA-COLI, Mutation, product inhibition, biology.protein, Bacillus circulans, lipids (amino acids, peptides, and proteins), site-directed mutagenesis, Cyclomaltodextrin glucanotransferase

Abstract

Cyclodextrin glycosyltransferase (CGTase) (EC 2.4.1.19) is used for the industrial production of cyclodextrins. Its application, however, is hampered by the limited cyclodextrin product specificity and the strong inhibitory effect of cyclodextrins on CGTase activity. Recent structural studies have identified Arg47 in the Bacillus circulans strain 251 CGTase as an active-site residue interacting with cyclodextrins, but not with linear oligosaccharides. Arg47 thus may specifically affect CGTase reactions with cyclic substrates or products.Here we show that mutations in Arg47 (to Leu or Gln) indeed have a negative effect on the cyclization and coupling activities; Arg47 specifically stabilizes the oligosaccharide chain in the transition state for these reactions. As a result, the mutant proteins display a shift in product specificity towards formation of larger cyclodextrins. As expected, both mutants also showed lower affinities for cyclodextrins in the coupling reaction, and a reduced competitive (product) inhibition of the disproportionation reaction by cyclodextrins.Both mutants also provide valuable information about the processes taking place during cyclodextrin production assays. Mutant Arg47-->Leu displayed an increased hydrolyzing activity, causing accumulation of increasing amounts of short oligosaccharides in the reaction mixture, which resulted in lower final amounts of cyclodextrins produced from starch. Interestingly, mutant Arg47-->Gln displayed an increased ratio of cyclization/coupling and a decreased hydrolyzing activity. Due to the decreased coupling activity, which especially affects the production of larger cyclodextrins, this CGTase variant produced the various cyclodextrins in a stable ratio in time. This feature is very promising for the industrial application of CGTase enzymes with improved product specificity.

Published

2000

36. The three transglycosylation reactions catalyzed by cyclodextrin glycosyltransferase from Bacillus circulans (strain 251) proceed via different kinetic mechanisms

Author

Gert-Jan W. M. van Alebeek, Bauke W. Dijkstra, Joost C.M. Uitdehaag, Lubbert Dijkhuizen, and Bart A. van der Veen

Subjects

Reaction rate, chemistry.chemical_classification, Cyclodextrin, Covalent bond, Stereochemistry, Chemistry, Substrate (chemistry), Disproportionation, Cyclodextrin glycosyltransferase, Biochemistry, Ternary complex, Coupling reaction

Abstract

Cyclodextrin glycosyltransferase (CGTase) catalyzes three transglycosylation reactions via a double displacement mechanism involving a covalent enzyme-intermediate complex (substituted-enzyme intermediate). Characterization of the three transglycosylation reactions, however, revealed that they differ in their kinetic mechanisms. Disproportionation (cleavage of an alpha-glycosidic bond of a linear malto-oligosaccharide and transfer of one part to an acceptor substrate) proceeds according to a ping-pong mechanism. Cyclization (cleavage of an alpha-glycosidic bond in amylose or starch and subsequent formation of a cyclodextrin) is a single-substrate reaction with an affinity for the high molecular mass substrate used, which was too high to allow elucidation of the kinetic mechanism. Michaelis-Menten kinetics, however, have been observed using shorter amylose chains. Coupling (cleavage of an alpha-glycosidic bond in a cyclodextrin ring and transfer of the resulting linear malto-oligosaccharide to an acceptor substrate) proceeds according to a random ternary complex mechanism. In view of the different kinetic mechanisms observed for the various reactions, which can be related to differences in substrate binding, it should be possible to mutagenize CGTase in such a manner that a single reaction is affected most strongly. Construction of CGTase mutants that synthesize linear oligosaccharides instead of cyclodextrins thus appears feasible. Furthermore, the rate of interconversion of linear and circular conformations of oligosaccharides in the cyclization and coupling reactions was found to determine the reaction rate. In the cyclization reaction this conversion rate, together with initial binding of the high molecular mass substrate, may determine the product specificity of the enzyme. These new insights will allow rational design of CGTase mutant enzymes synthesizing cyclodextrins of specific sizes.

Published

2000

37. The Cyclization Mechanism of Cyclodextrin Glycosyltransferase (CGTase) as Revealed by a γ-Cyclodextrin-CGTase Complex at 1.8-Å Resolution

Author

Joost C.M. Uitdehaag, Lubbert Dijkhuizen, Bart A. van der Veen, Bauke W. Dijkstra, Kor H. Kalk, X-ray Crystallography, and Host-Microbe Interactions

Subjects

Models, Molecular, Protein Conformation, Stereochemistry, Mutant, Oligosaccharides, Bacillus, Cyclodextrin glycosyltransferase, Biochemistry, Protein structure, Bacterial Proteins, polycyclic compounds, Transferase, Binding site, Molecular Biology, chemistry.chemical_classification, Cyclodextrins, Binding Sites, Cyclodextrin, Chemistry, Mutagenesis, technology, industry, and agriculture, Cell Biology, carbohydrates (lipids), Enzyme, Glucosyltransferases, lipids (amino acids, peptides, and proteins), alpha-Amylases, gamma-Cyclodextrins

Abstract

The enzyme cyclodextrin glycosyltransferase is closely related to alpha-amylases but has the unique ability to produce cyclodextrins (circular alpha(1-->4)-linked glucoses) from starch. To characterize this specificity we determined a 1.8-A structure of an E257Q/D229N mutant cyclodextrin glycosyltransferase in complex with its product gamma-cyclodextrin, which reveals for the first time how cyclodextrin is competently bound. Across subsites -2, -1, and +1, the cyclodextrin ring binds in a twisted mode similar to linear sugars, giving rise to deformation of its circular symmetry. At subsites -3 and +2, the cyclodextrin binds in a manner different from linear sugars. Sequence comparisons and site-directed mutagenesis experiments support the conclusion that subsites -3 and +2 confer the cyclization activity in addition to subsite -6 and Tyr-195. On this basis, a role of the individual residues during the cyclization reaction cycle is proposed.

Published

1999

38. [Untitled]

Author

Lubbert Dijkhuizen, Joost C.M. Uitdehaag, Kor H. Kalk, Bauke W. Dijkstra, Stephen G. Withers, Renee Mosi, and Bart A. van der Veen

Subjects

biology, Hydrogen bond, Chemistry, Stereochemistry, Active site, Substrate (chemistry), Cyclodextrin glycosyltransferase, Reaction intermediate, Biochemistry, Catalysis, Crystallography, Protein structure, Structural Biology, Covalent bond, Genetics, biology.protein

Abstract

Cyclodextrin glycosyltransferase (CGTase) is an enzyme of the α-amylase family, which uses a double displacement mechanism to process α-linked glucose polymers. We have determined two X-ray structures of CGTase complexes, one with an intact substrate at 2.1 A resolution, and the other with a covalently bound reaction intermediate at 1.8 A resolution. These structures give evidence for substrate distortion and the covalent character of the intermediate and for the first time show, in atomic detail, how catalysis in the α-amylase family proceeds by the concerted action of all active site residues.

Published

1999

39. General Model for Lipid-Mediated Two-Dimensional Array Formation of Membrane Proteins: Application to Bacteriorhodopsin

Author

Anthony Watts, Joost C.M. Uitdehaag, and Mads C. Sabra

Subjects

Models, Molecular, Macromolecular Substances, Lipid Bilayers, Biophysics, Plasma protein binding, Biophysical Phenomena, Computer Simulation, cardiovascular diseases, Lipid bilayer, biology, Chemistry, Membrane Proteins, Bacteriorhodopsin, Atmospheric temperature range, Crystallography, Membrane protein, Chemical physics, Bacteriorhodopsins, Excited state, cardiovascular system, biology.protein, Thermodynamics, lipids (amino acids, peptides, and proteins), Ground state, Monte Carlo Method, Protein Binding, Research Article

Abstract

Based on experimental evidence for 2D array formation of bacteriorhodopsin, we propose a general model for lipid-mediated 2D array formation of membrane proteins in lipid bilayers. The model includes two different lipid species, “annular” lipids and “neutral” lipids, and one protein species. The central assumption of the model is that the annular lipids interact more strongly with the protein than with the neutral lipids. Monte Carlo simulations performed on this model show that 2D arrays of proteins only form when there are annular lipids present. In addition, no arrays form if all of the lipids present are annular lipids. The geometry of the observed arrays is for the most part hexagonal. However, for a certain range of low annular lipid/protein ratios, arrays form that have geometries other than hexagonal. Using the assumption that the hydrocarbon chains of the annular lipids are restricted in motion when close to a protein, we expand the model to include a ground state and an excited state of the annular lipids. The main result from the extended model is that within a certain temperature range, increasing the temperature will lead to larger and more regular protein arrays.

Published

1998

40. Comparison of the cancer gene targeting and biochemical selectivities of all targeted kinase inhibitors approved for clinical use

Author

Martine B.W. Prinsen, Joost C.M. Uitdehaag, Jeroen A.D.M. de Roos, Yoshinori Tanizawa, R.C. Buijsman, Guido J.R. Zaman, Yusuke Kawase, Kohichiro Yoshino, Jos de Man, and Antoon M. van Doornmalen

Subjects

Drug, Genetic Markers, Drug Research and Development, Proteome, media_common.quotation_subject, Cancer Treatment, lcsh:Medicine, Drug action, Biology, Pharmacology, Biochemistry, Cell Growth, Neoplasms, Chemical Biology, Molecular Cell Biology, Drug Discovery, Medicine and Health Sciences, Humans, Kinome, lcsh:Science, Protein Kinase Inhibitors, media_common, EGFR inhibitors, Trametinib, Analysis of Variance, Multidisciplinary, ABL, Cell Death, Kinase, Drug discovery, lcsh:R, Reproducibility of Results, Biology and Life Sciences, Cell Biology, Enzymes, Chemistry, Oncology, Small Molecules, Cell Processes, Gene Targeting, Physical Sciences, Enzymology, lcsh:Q, Oncology Agents, Antiangiogenesis Therapy, Clinical Medicine, Research Article, Biotechnology

Abstract

The anti-proliferative activities of all twenty-five targeted kinase inhibitor drugs that are in clinical use were measured in two large assay panels: (1) a panel of proliferation assays of forty-four human cancer cell lines from diverse tumour tissue origins; and (2) a panel of more than 300 kinase enzyme activity assays. This study provides a head-on comparison of all kinase inhibitor drugs in use (status Nov. 2013), and for six of these drugs, the first kinome profiling data in the public domain. Correlation of drug activities with cancer gene mutations revealed novel drug sensitivity markers, suggesting that cancers dependent on mutant CTNNB1 will respond to trametinib and other MEK inhibitors, and cancers dependent on SMAD4 to small molecule EGFR inhibitor drugs. Comparison of cellular targeting efficacies reveals the most targeted inhibitors for EGFR, ABL1 and BRAF(V600E)-driven cell growth, and demonstrates that the best targeted agents combine high biochemical potency with good selectivity. For ABL1 inhibitors, we computationally deduce optimized kinase profiles for use in a next generation of drugs. Our study shows the power of combining biochemical and cellular profiling data in the evaluation of kinase inhibitor drug action.

Published

2013

41. Abstract 2646: The unique binding mode of NTRC 0066-0, a novel inhibitor of the spindle assembly checkpoint kinase TTK (Mps1), leads to long target residence time and potent antitumor activity

Author

Jeroen A.D.M. de Roos, Martine B.W. Prinsen, Guido J.R. Zaman, Joost C.M. Uitdehaag, Rogier C. Buijsman, Joeri Johannes Petrus De Wit, Jos de Man, Nicole Willemsen-Seegers, and Jan Gerard Sterrenburg

Subjects

Cancer Research, biology, Chemistry, Kinase, Cell cycle, Cell biology, Spindle checkpoint, Oncology, Protein kinase domain, Biochemistry, Cyclin-dependent kinase, biology.protein, Kinase activity, Protein kinase A, Mitosis

Abstract

[purpose] An abnormal number of chromosomes, or ‘aneuploidy’, is a common feature of solid human tumors and a predictor of poor prognosis in breast, lung, brain and colorectal cancer. Aneuploidy is caused by malfunctioning of the Spindle Assembly Checkpoint (SAC), a surveillance mechanism that ensures the fidelity of chromosome segregation. The protein kinase TTK (commonly referred to as Mps1) is a component of the SAC. Inhibition of TTK gene expression by RNA interference and inhibition of TTK kinase activity by small molecule kinase inhibitors causes chromosome missegregation and cancer cell death. [experimental procedures] A novel class of compounds was identified that potently inhibits TTK enzyme activity and cancer cell line proliferation [1]. Its binding mode and that of reference inhibitors was characterized by protein crystallography. Binding kinetics and target residence time were determined by surface plasmon resonance using Biacore T200. Anti-proliferative activity was measured on a broad panel of cancer cell lines [2]. [results] The clinical candidate, NTRC 0066-0, inhibits TTK with subnanomolar potency (IC50) in a kinase enzyme assay and is more than 200 times selective over 276 kinases examined, including mitotic and cell cycle dependent kinases (CDKs). X-ray structures of the TTK kinase domain in complex with NTRC 0066-0 and analogs indicate that this class of compounds induces a large conformational shift in the glycine-rich loop, invoking an inactive kinase conformation. In surface plasmon resonance experiments, NTRC 0066-0 exhibited slow dissociation kinetics, resulting in a long target residence time. Parallel surface plasmon resonance experiments with mitotic kinases confirmed the exquisite selectivity of NTRC 0066-0 for TTK over Aurora and Polo-like kinases. NTRC 0066-0 potently inhibited the proliferation of a wide variety of human cancer cell lines with potencies in the same range as marketed cytotoxic agents. The crystal structure, binding kinetics and cellular potency of NTRC 0066-0 were compared to that of other TTK inhibitors such as Mps1-IN-2, AZD-3146, Mps-BAY2b and Bay 1161909 as well as analogs from the NTRC 0066-0 series. This suggest that the unique binding mode of NTRC 0066-0 results in long target residence time which contributes to its strong anti-tumor activity. In subsequent mouse xenograft models of human cancer cell lines, NTRC 0066-0 inhibited tumor growth as a single agent after oral administration at 20 mg per kg. [conclusions] NTRC 0066-0 is a novel TTK inhibitor with outstanding in vitro properties and potent anti-tumor activity in mouse xenograft models. Our data suggest that long target residence time corresponds with potent cellular activity for TTK inhibitors. References [1] Maia et al. (2015) Annals of Oncology 26, 2180-2192; [2] Uitdehaag et al. (2014) PLOS ONE 9(3) e92146. Citation Format: Jos de Man, Joost C.M. Uitdehaag, Nicole Willemsen-Seegers, Jan Gerard Sterrenburg, Joeri J.P. de Wit, Jeroen A.D.M. de Roos, Martine B.W. Prinsen, Rogier C. Buijsman, Guido J.R. Zaman. The unique binding mode of NTRC 0066-0, a novel inhibitor of the spindle assembly checkpoint kinase TTK (Mps1), leads to long target residence time and potent antitumor activity. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 2646.

Published

2016

42. Abstract 4635: Comparative cancer cell line profiling differentiates the mechanism of action of different PI3K/mTOR, Aurora kinase and EZH2 inhibitors

Author

Jeroen A.D.M. de Roos, Rogier C. Buijsman, Judith R.F. de Vetter, Jos de Man, Guido J.R. Zaman, Suzanne J.C. van Gerwen, Joost C.M. Uitdehaag, Jelle Dylus, Antoon M. van Doornmalen, and Martine B.W. Prinsen

Subjects

Cancer Research, Aurora kinase, ABL, Oncology, Kinase, Cancer cell, Cancer research, Aurora inhibitor, biology.protein, Bruton's tyrosine kinase, Biology, PI3K/AKT/mTOR pathway, EGFR inhibitors

Abstract

[purpose] Profiling of drug candidates in cell line panels is an important tool to compare the selectivity and targeting of new anti-cancer agents. In addition, comparative profiling may be used to repurpose established therapeutics by identifying new mechanisms of action or cross-selectivities. [experimental procedures] A collection of more than 120 anti-cancer agents, targeting all important oncogenic signaling pathways, including classic cytotoxic agents as well as many targeted kinase inhibitors and epigenetic modulators, was profiled on a panel of 44 or 66 parallel cell line proliferation assays (Oncolines™) [1,2]. The Oncolines™ profiles of the compounds were compared by Pearson correlations of their inhibitor responses. Inhibitor sets were clustered using hierarchical trees. Response profiles were correlated to the genetic background of the cell lines by Analysis of Variance (Anova). [results] Reproducibility of the NTRC Oncolines™ cell panel was validated by monitoring cell growth rate and the variation in IC50s of replicate profiles over a period of three years. The Pearson correlation between replicates ranged between 0.60 and 0.99 for 16 different inhibitors, depending on dose-response curve shape. Correlation analyses of the > 120 profiled anti-cancer agents revealed separate clusters of, a.o., taxanes, platins, topo-isomerase inhibitors, and EGFR, ABL, MEK and BRAF inhibitors. This demonstrates that the Oncolines™ profiles are an unbiased representation of the compound's mechanisms. The profile of the BTK inhibitor ibrutinib correlated with EGFR inhibitors. In biochemical experiments we showed that this due to its cross-reactivity with EGFR. The six Aurora kinase inhibitors profiled fall into two separate clusters, which are related to their biochemical selectivity. Thus, Aurora A-selective inhibitors are relatively more active in cell lines with mutations in cell cycle checkpoint-related genes such as TP53 and RB1; whereas pan-Aurora inhibitors are more active in cell lines with mutations in growth factor signaling pathways, such as NRAS. Profiling of eleven PI3 kinase and mTOR inhibitors revealed four distinct clusters. PI3Kalpha and PI3Kdelta isoform selective inhibitors each target genetically distinct subgroups of cell lines. Rapamycin-analogs, such as everolimus, specifically target PTEN-mutant cell lines. Finally, profiling of EZH2 inhibitors indicates that there are essentially two classes and that these have a cellular profile that is distinct from HDAC, DOT1L or BET inhibitors. [conclusions] Comparative cancer cell line profiling is a powerful tool to rapidly explore the pharmacogenomics of drug action in cancer cells and to identify new or previously unnoted activities of compounds. [references]: [1] Uitdehaag et al. (2014) PLOS ONE 9(3) e92146; [2] Uitdehaag et al. (2015) PLOS ONE 10(6) e0132230. Citation Format: Joost C.M. Uitdehaag, Jeroen A.D.M. de Roos, Martine B.W. Prinsen, Judith R.F. de Vetter, Jelle Dylus, Antoon M. van Doornmalen, Suzanne J.C. van Gerwen, Jos de Man, Rogier C. Buijsman, Guido J.R. Zaman. Comparative cancer cell line profiling differentiates the mechanism of action of different PI3K/mTOR, Aurora kinase and EZH2 inhibitors. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 4635.

Published

2016

43. Bet hedging based cooperation can limit kin selection and form a basis for mutualism

Author

Joost C.M. Uitdehaag

Subjects

Statistics and Probability, Mutualism (biology), General Immunology and Microbiology, Reproductive success, Models, Genetic, Ecology, Applied Mathematics, Inclusive fitness, General Medicine, Kin selection, Biology, General Biochemistry, Genetics and Molecular Biology, Microeconomics, Evolution, Molecular, Parochialism, Modeling and Simulation, Mutation, Animals, Reciprocal altruism, Selection, Genetic, General Agricultural and Biological Sciences

Abstract

Mutualism is a mechanism of cooperation in which partners that differ help each other. As such, mutualism opposes mechanisms of kin selection and tag-based selection (for example the green beard mechanism), which are based on giving exclusive help to partners that are related or carry the same tag. In contrast to kin selection, which is a basis for parochialism and intergroup warfare, mutualism can therefore be regarded as a mechanism that drives peaceful coexistence between different groups and individuals. Here the competition between mutualism and kin (tag) selection is studied. In a model where kin selection and tag-based selection are dominant, mutualism is promoted by introducing environmental fluctuations. These fluctuations cause reduction in reproductive success by the mechanism of variance discount. The best strategy to counter variance discount is to share with agents who experience the most anticorrelated fluctuations, a strategy called bet hedging. In this way, bet hedging stimulates cooperation with the most unrelated partners, which is a basis for mutualism. Analytic results and simulations reveal that, if this effect is large enough, mutualistic strategies can dominate kin selective strategies. In addition, mutants of these mutualistic strategies that experience fluctuations that are more anticorrelated to their partner, can outcompete wild type, which can lead to the evolution of specialization. In this way, the evolutionary success of mutualistic strategies can be explained by bet hedging-based cooperation.

Published

2010

44. Dioxo-triazines as a novel series of cathepsin K inhibitors

Author

Sylviane Boucharens, Joost C.M. Uitdehaag, Jonathan Gillespie, Mario van Zeeland, Zoran Rankovic, Jiaqiang Cai, Maureen Dempster, Clive Long, Iain Cumming, Ann Mitchell, Emma Hamilton, Ashvin Mistry, Craig Jamieson, Angela King, and X. Fradera

Subjects

Stereochemistry, Clinical Biochemistry, Cathepsin K, Pharmaceutical Science, Cathepsin E, Cathepsin F, Cysteine Proteinase Inhibitors, Crystallography, X-Ray, Biochemistry, Cathepsin A, Cathepsin B, Cathepsin L, Structure-Activity Relationship, Cathepsin O, Cathepsin H, Cathepsin L1, Catalytic Domain, Drug Discovery, Humans, Uracil, Molecular Biology, Binding Sites, biology, Chemistry, Triazines, Organic Chemistry, High-Throughput Screening Assays, biology.protein, Molecular Medicine

Abstract

A novel dioxo-triazine series of cathepsin K inhibitors was identified from HTS. A rapid exploratory programme led to the discovery of potent and selective cathepsin K inhibitors, typified by compound 24 which displayed IC(50) values of 17nM against catK and10,000nM in catL, catB and catS assays.

Published

2009

45. The X-ray Structure of RU486 Bound to the Progesterone Receptor in a Destabilized Agonistic Conformation

Author

Hans C. A. Raaijmakers, Judith E. Versteegh, and Joost C.M. Uitdehaag

Subjects

Agonist, Models, Molecular, endocrine system, medicine.drug_class, Stereochemistry, Protein Conformation, Dimer, Molecular Conformation, Crystal structure, Crystallography, X-Ray, Biochemistry, Protein Structure, Secondary, chemistry.chemical_compound, Protein structure, Hormone Antagonists, Receptors, Glucocorticoid, Progesterone receptor, medicine, polycyclic compounds, Humans, Binding site, Molecular Biology, Binding Sites, Molecular Structure, Chemistry, Cell Biology, Ligand (biochemistry), Protein Structure, Tertiary, Crystallography, Mifepristone, Helix, Protein Structure and Folding, Receptors, Progesterone, hormones, hormone substitutes, and hormone antagonists

Abstract

Here we describe the 1.95 A structure of the clinically used antiprogestin RU486 (mifepristone) in complex with the progesterone receptor (PR). The structure was obtained by taking a crystal of the PR ligand binding domain containing the agonist norethindrone and soaking it in a solution containing the antagonist RU486 for extended times. Clear ligand exchange could be observed in one copy of the PR ligand binding domain dimer in the crystal. RU486 binds while PR is in an agonistic conformation without displacing helix 12. Although this is probably because of the constraints of the crystal lattice, it demonstrates that helix 12 displacement is not a prerequisite for RU486 binding. Interestingly, B-factor analysis clearly shows that helix 12 becomes more flexible after RU486 binding, suggesting that RU486, being a model antagonist, does not induce one fixed conformation of helix 12 but changes its positional equilibrium. This conclusion is confirmed by comparing the structures of RU486 bound to PR and RU486 bound to the glucocorticoid receptor.

Published

2009

46. Managing freedom: managing researchers as if they were warriors

Author

Joost C.M. Uitdehaag

Subjects

Pharmacology, Motivation, Drug Industry, Drug Discovery, Professional Autonomy, Sociology, Efficiency, Organizational, Personnel Management, Research Personnel

Published

2008

47. 3D Modeling of Novel Transforming JAK Mutations in T-Cell Acute Lymphoblastic Leukemia Reveals Altered Pseudokinase-Kinase Domain Interactions That Result in Constitutive JAK Kinase Activity

Author

Guido J.R. Zaman, Wilco K Smits, Rob Pieters, Kirsten Canté-Barrett, Rogier C. Buijsman, Jessica Buijs-Gladdines, Joost C.M. Uitdehaag, and Jules P.P. Meijerink

Subjects

Genetics, Mutation, Kinase, Immunology, Wild type, Cell Biology, Hematology, Biology, medicine.disease_cause, Biochemistry, Protein kinase domain, Tyrosine kinase 2, medicine, Kinase activity, Janus kinase, Protein kinase B

Abstract

Background: Many pediatric T-cell acute lymphoblastic leukemia patients harbor mutations in IL7Ra or downstream molecules encoded by JAK1, JAK3, N-RAS, K-RAS, NF1, AKT, and PTEN. These mutated signaling molecules can contribute to leukemia by disturbing a multitude of cellular processes such as the cell cycle, epigenetics, apoptosis, or affecting other important signal transduction pathways. Aims: We aimed to determine the overall incidence of JAK family mutations in a large cohort of T-ALL patients. We also aimed to generate a 3D JAK1 model including known and newly identified JAK mutations in order to better understand how these contribute to JAK kinase activity and the transformation of cells. Methods: We screened 146 pediatric T-ALL patient samples for mutations in the FERM, pseudokinase and kinase domains of the Janus kinase gene family (JAK1-3, TYK2). To establish a 3D JAK1 model, we superimposed individual pseudokinase and kinase crystallographic structures on the homologous TYK2 pseudokinase-kinase structure. We visualized JAK mutations and their effects on the 3D structure. We modified the IL3-dependent Ba/F3 cell line to express JAK mutant or wild type genes upon induction by doxycycline. We tested these Ba/F3 derivative lines for transforming ability, signaling, and resistance to various inhibitors in the absence of IL3. Results: JAK1 or JAK3 mutations were found in 10 patients; no mutations were found in JAK2 or TYK2. We found JAK1 and JAK3 mutations as previously reported, but also identified amino acid substitutions as a result of novel JAK1 mutations including V427M, L624YPILKV, E668Q, P815S, and T901G. Our novel 3D model of JAK1 places most mutations in one of two crucial pseudokinase-kinase interaction sites, which can weaken the interaction and facilitate constitutive kinase activity. One interaction is between the hinge region of the pseudokinase domain and the loop in the kinase domain, which is supported by four salt bridges. Mutations in T-ALL disrupting these salt bridges include E668Q, R724H and its JAK3 equivalent R657Q, and T901G. The second interaction with the kinase domain is formed by a helical domain in the pseudokinase domain, located just upstream of the conserved F575-F636-V658 triad. This F-F-V triad is predicted to act as a structural switch that controls the catalytic activity of JAK kinases. Various mutations occur in the direct vicinity and can affect the function of this switch. V658F in T-ALL and its JAK2 equivalent V617F in polycythemia vera patients are mutations in this triad. The frequent JAK3 mutation M511I in T-ALL flanks the F513 residue (equivalent of JAK1 F575) and also affects the F-F-V triad. The L624YPILKV insertion mutation is located in a loop near the helical domain, which may also subtly compromise the F-F-V triad structural switch leading to derepression of the kinase domain. Expression of mutant JAK genes-in contrast to the wild type genes-transforms Ba/F3 cells by supporting IL3-independent growth, and by activating downstream RAS-MEK-ERK and PI3K-AKT pathways. This pathway activation as a result of ligand-independent mutant JAK kinase activity was confirmed by measuring phospho-proteins including p-MEK, p-ERK, p-AKT, p-mTOR, and p-p70S6K, and can be blocked by JAK inhibitors. Notably, JAK3 mutants signal significantly weaker than JAK1 mutants, possibly due to different dependence on (endogenous) receptors that normally mediate wild type JAK signaling. Summary/Conclusion: In a 3D model, we show that JAK mutations are located in critical interface regions between the pseudokinase and kinase domains, maintaining the kinase in an open, active confirmation. The inducible Ba/F3 model system confirms the transforming capacity of JAK mutations, reveals constitutive active downstream signaling, and is also suitable to test the effect of various inhibitors. The visualization of various JAK mutations in a 3D model and how these contribute to kinase activity provides insight in how mutant JAK could be inhibited, helping guide the development of new small molecule inhibitors of mutant JAKs. Disclosures Buijsman: Netherlands Translational Research Center B.V.: Equity Ownership, Other: founder and shareholder. Zaman:Netherlands Translational Research Center B.V.: Equity Ownership, Other: founder and shareholder.

Published

2015

48. Abstract 3502: Selective targeting of CTNBB1-, KRAS- or MYC-driven cell growth by combinations of existing drugs

Author

Jill A.P. Spijkers Hagelstein, Guido J.R. Zaman, Jeroen A.D.M. de Roos, Joost C.M. Uitdehaag, Antoon M. van Doornmalen, Rogier C. Buijsman, Judith R.F. de Vetter, Jos de Man, and Martine B.W. Prinsen

Subjects

Trametinib, Genetics, Cancer Research, Cell growth, MEK inhibitor, Aurora inhibitor, Dabrafenib, Biology, medicine.disease_cause, Oncology, Neratinib, Cancer cell, medicine, Cancer research, KRAS, medicine.drug

Abstract

Purpose: Combination therapy plays an important role in achieving durable responses in anticancer therapy. Ideally, compound combinations work synergistically in cancer cells and not in non-malignant cells. Here we present a rational approach for identifying pairs of selective inhibitors that show a synergistic interaction only in specific genetic backgrounds, i.e. mutated in the CTNNB1 (β-catenin) or KRAS genes, or expressing amplified MYC. Experimental Procedures: We have established a panel of sixty six genetically well-characterized cell lines that represents the most frequently occurring oncogenic drivers in cancer (1). A collection of more than 100 inhibitors targeting all important oncogenic signaling pathways, including many kinase and epigenetic regulators, was profiled in a subset of forty four cell lines, generating highly reproducible and high-quality cell proliferation data. The inhibitor response was correlated to the genetic background of the cell lines by Anova analysis (1). Compounds that targeted similar subsets of cell lines, were tested in combination for synergistic interaction, using in vitro proliferation assays with equipotent mixtures, followed by curve shift analysis, isobolograms and combination index scoring. The approach was validated by showing that the MEK inhibitor trametinib and the BRAF inhibitor dabrafenib, which are targeted to BRAF-mutant cell lines, show synergistic interaction in this subpopulation, and not in other cell line types. Results: For all inhibitors, the drug response in cell line panel (Oncolines™) was analyzed. Notably, the Wnt-pathway inhibitor ICG-001 and the MEK inhibitor trametinib were shown to preferentially inhibit CTNNB1-mutated cancer cell lines. Neratinib, a spectrum selective EGFR inhibitor, and GSK-1070916, an Aurora kinase inhibitor, were shown to target MYC-amplified cell lines. The ERBB2 inhibitor TAK-165 and trametinib targeted KRAS mutant cell lines. These compounds thus show a pharmacological synthetic lethal effect. Subsequent combination studies showed synergy on cell proliferation in a high number of cases. ICG-001 works synergistically with trametinib in a CTNNB1-mutant colon cell line, and not in CTNNB1-wild type colon cell lines. Neratinib and GSK-1070916 work synergistically in MYC-amplified cell lines and not in non-MYC-amplified lines. Conclusions: Pharmacogenomic analysis of single agent responses identified compounds that preferentially inhibit the growth of cell lines harbouring mutant CTNNB1 or KRAS, or amplified MYC. Synergy studies in the pertinent genetic background identified new combinations of existing drugs with enhanced targeting of CTNNB1-mutated or MYC-amplified cancer cell lines. Our approach can efficiently discover novel drug combinations that target cancer genes more selectively and more potently. References: 1. Uitdehaag et al. (2014) PLOS ONE 9(3) e92146. Citation Format: Joost C.M. Uitdehaag, Jeroen A.D.M. de Roos, Antoon M. van Doornmalen, Martine B.W. Prinsen, Jill A.P. Spijkers - Hagelstein, Judith R.F. de Vetter, Jos de Man, Rogier C. Buijsman, Guido J.R. Zaman. Selective targeting of CTNBB1-, KRAS- or MYC-driven cell growth by combinations of existing drugs. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 3502. doi:10.1158/1538-7445.AM2015-3502

Published

2015

49. Where is the optimism? Warrior teachings to regain the drug discovery spirit

Author

Joost C.M. Uitdehaag

Subjects

Pharmacology, Optimism, Psychotherapist, Drug Industry, Drug discovery, media_common.quotation_subject, Political science, Drug Design, Drug Discovery, Humans, Technology, Pharmaceutical, Research Personnel, media_common

Published

2006

50. Crystal structure of the CUB1-EGF-CUB2 region of mannose-binding protein associated serine protease-2

Author

Hadar Feinberg, Russell Wallis, Joost C.M. Uitdehaag, Kurt Drickamer, Jason M Davies, and William I. Weis

Subjects

Models, Molecular, Proteases, Materials science, Protein Conformation, medicine.medical_treatment, Molecular Sequence Data, CHO Cells, Calorimetry, Crystallography, X-Ray, Mannose-Binding Lectin, General Biochemistry, Genetics and Molecular Biology, Serine, Cricetinae, Hydrolase, medicine, Animals, Humans, Amino Acid Sequence, Molecular Biology, Serine protease, Protease, General Immunology and Microbiology, biology, General Neuroscience, Serine Endopeptidases, Articles, CUB domain, Complement system, Cell biology, Rats, Biochemistry, Mannose-Binding Protein-Associated Serine Proteases, biology.protein, Calcium, Dimerization, Sequence Alignment, Complement control protein, Protein Binding

Abstract

Serum mannose-binding proteins (MBPs) are C-type lectins that recognize cell surface carbohydrate structures on pathogens, and trigger killing of these targets by activating the complement pathway. MBPs circulate as a complex with MBP-associated serine proteases (MASPs), which become activated upon engagement of a target cell surface. The minimal functional unit for complement activation is a MASP homodimer bound to two MBP trimeric subunits. MASPs have a modular structure consisting of an N-terminal CUB domain, a Ca(2+)-binding EGF-like domain, a second CUB domain, two complement control protein modules and a C-terminal serine protease domain. The CUB1-EGF-CUB2 region mediates homodimerization and binding to MBP. The crystal structure of the MASP-2 CUB1-EGF-CUB2 dimer reveals an elongated structure with a prominent concave surface that is proposed to be the MBP-binding site. A model of the full six-domain structure and its interaction with MBPs suggests mechanisms by which binding to a target cell transmits conformational changes from MBP to MASP that allow activation of its protease activity.

Published

2003