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52. Identification and Characterization of NVP-BKM120, an Orally Available Pan-Class I PI3-Kinase Inhibitor

Author

Marion Dorsch, Daniel Guthy, Sauveur-Michel Maira, Robert Schlegel, Tobi Nagel, Alan Huang, Dario Sterker, Charles Voliva, Alain De Pover, Carlos Garcia-Echeverria, Marion Wiesmann, Georg Martiny-Baron, Patrick Chène, Sabina Pecchi, Christine Fritsch, Doriano Fabbro, Saskia M. Brachmann, Christian Schnell, Christine D. Wilson, Mark Knapp, Daniel Menezes, Matthew Burger, Kevin Shoemaker, William R. Sellers, and Francesco Hofmann

Subjects
Models, Molecular, Cancer Research, Morpholines, Blotting, Western, Buparlisib, Administration, Oral, Aminopyridines, Biological Availability, Mice, Nude, Biology, Pharmacology, medicine.disease_cause, Mice, chemistry.chemical_compound, In vivo, Cell Line, Tumor, Neoplasms, medicine, Animals, Humans, PTEN, Cytotoxicity, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Phosphoinositide-3 Kinase Inhibitors, Mutation, Dose-Response Relationship, Drug, Molecular Structure, Kinase, HCT116 Cells, Xenograft Model Antitumor Assays, Protein Structure, Tertiary, Rats, Tumor Burden, Isoenzymes, Oncology, Mechanism of action, chemistry, biology.protein, Phosphatidylinositol 3-Kinase, medicine.symptom, HT29 Cells, Proto-Oncogene Proteins c-akt, Protein Binding
Abstract

Following the discovery of NVP-BEZ235, our first dual pan-PI3K/mTOR clinical compound, we sought to identify additional phosphoinositide 3-kinase (PI3K) inhibitors from different chemical classes with a different selectivity profile. The key to achieve these objectives was to couple a structure-based design approach with intensive pharmacologic evaluation of selected compounds during the medicinal chemistry optimization process. Here, we report on the biologic characterization of the 2-morpholino pyrimidine derivative pan-PI3K inhibitor NVP-BKM120. This compound inhibits all four class I PI3K isoforms in biochemical assays with at least 50-fold selectivity against other protein kinases. The compound is also active against the most common somatic PI3Kα mutations but does not significantly inhibit the related class III (Vps34) and class IV (mTOR, DNA-PK) PI3K kinases. Consistent with its mechanism of action, NVP-BKM120 decreases the cellular levels of p-Akt in mechanistic models and relevant tumor cell lines, as well as downstream effectors in a concentration-dependent and pathway-specific manner. Tested in a panel of 353 cell lines, NVP-BKM120 exhibited preferential inhibition of tumor cells bearing PIK3CA mutations, in contrast to either KRAS or PTEN mutant models. NVP-BKM120 shows dose-dependent in vivo pharmacodynamic activity as measured by significant inhibition of p-Akt and tumor growth inhibition in mechanistic xenograft models. NVP-BKM120 behaves synergistically when combined with either targeted agents such as MEK or HER2 inhibitors or with cytotoxic agents such as docetaxel or temozolomide. The pharmacological, biologic, and preclinical safety profile of NVP-BKM120 supports its clinical development and the compound is undergoing phase II clinical trials in patients with cancer. Mol Cancer Ther; 11(2); 317–28. ©2011 AACR.

Published
2012
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53. Factors influencing the inhibition of protein kinases

Author

Patrick Chène, Jean-Christophe Hau, Dirk Erdmann, Alain De Pover, Marielle Brockhoff, Catherine Zimmermann, and Patrizia Fontana

Subjects
Protein Conformation, Cofactor, Receptor, IGF Type 1, Substrate Specificity, chemistry.chemical_compound, Adenosine Triphosphate, Growth factor receptor, Drug Discovery, Humans, Potency, Magnesium, Pyrroles, Enzyme Inhibitors, Protein kinase A, Protein Kinase Inhibitors, Magnesium ion, Insulin-like growth factor 1 receptor, Pharmacology, biology, Kinase, General Medicine, Staurosporine, Peptide Fragments, Kinetics, Pyrimidines, chemistry, Biochemistry, biology.protein, Protein Kinases, Adenosine triphosphate
Abstract

The protein kinase field is a very active research area in the pharmaceutical industry and many activities are ongoing to identify inhibitors of these proteins. The design of new chemical entities with improved pharmacological properties requires a deeper understanding of the factors that modulate inhibitor-kinase interactions. In this report, we studied the effect of two of these factors--the magnesium ion cofactor and the protein substrate--on inhibitors of the type I insulin-like growth factor receptor. Our results show that the concentration of magnesium ion influences the potency of adenosine triphosphate (ATP) competitive inhibitors, suggesting an explanation for the observation that such compounds retain their nanomolar potency in cells despite the presence of millimolar levels of ATP. We also showed that the peptidic substrate affects the potency of these inhibitors in a different manner, suggesting that the influence of this substrate on compound potency should be taken into consideration during drug discovery.

Published
2011
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54. Kinetic Study of Human Full-Length Wild-Type JAK2 and V617F Mutant Proteins

Author

Jacqueline Bohn, Alain De Pover, Andreas Floersheimer, Patrizia Fontana, Dirk Erdmann, Bertrand Allard, Patrick Chène, Marc Gerspacher, Francesco Hofmann, Jean Christophe Hau, Thomas Radimerski, Roman Wille, and Catherine Zimmermann

Subjects
Janus kinase 2, biology, Chemistry, Drug target, Mutant, Wild type, food and beverages, Molecular biology, Protein kinase domain, hemic and lymphatic diseases, Mutation (genetic algorithm), biology.protein, Missense mutation, Gene, hormones, hormone substitutes, and hormone antagonists
Abstract

The Janus kinase 2 (JAK2) is a drug target in particular because a missense mutation in this gene (V617F) has been identified in various human diseases. We report here the first kinetic study of the human full-length wild type and V617F JAK2 proteins and of their isolated kinase domain. The kinetic parameters of both full-length proteins are similar revealing that the mutation does not affect JAK2 catalytic activity suggesting that it has a more complex role in the regu- lation of JAK2 activity. Our study also shows that the domains located outside the kinase domain have little influence on JAK2 catalytical activity.

Published
2009
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55. Characterization of the novel and specific PI3Kα inhibitor NVP-BYL719 and development of the patient stratification strategy for clinical trials

Author

Pascal Furet, Joseph Lehar, Alain De Pover, Christine D. Wilson, Manway Liu, Daniel Guthy, Sauveur-Michel Maira, Dirk Erdmann, Anupama Reddy, Joerg Trappe, Patrick Chène, Stephane Ferretti, Audrey Kauffmann, William R. Sellers, Robert Schlegel, Youzhen Wang, Giorgio Caravatti, Christine Fritsch, Christian Schnell, Markus Boehm, Hui Gao, Robert Cozens, Christian Chatenay-Rivauday, Saskia M. Brachmann, Francesco Hofmann, Alan Huang, Carlos Garcia-Echeverria, and Marion Wiesmann

Subjects
Cancer Research, Class I Phosphatidylinositol 3-Kinases, Buparlisib, Drug Evaluation, Preclinical, Antineoplastic Agents, Disease, medicine.disease_cause, Bioinformatics, chemistry.chemical_compound, Inhibitory Concentration 50, Mice, Phosphatidylinositol 3-Kinases, In vivo, Cell Line, Tumor, Neoplasms, medicine, PTEN, Animals, Humans, PI3K/AKT/mTOR pathway, Phosphoinositide-3 Kinase Inhibitors, Mutation, biology, PTEN Phosphohydrolase, Xenograft Model Antitumor Assays, Rats, Clinical trial, Disease Models, Animal, Thiazoles, Oncology, Tolerability, chemistry, Drug Resistance, Neoplasm, biology.protein, Cancer research, Female
Abstract

Somatic PIK3CA mutations are frequently found in solid tumors, raising the hypothesis that selective inhibition of PI3Kα may have robust efficacy in PIK3CA-mutant cancers while sparing patients the side-effects associated with broader inhibition of the class I phosphoinositide 3-kinase (PI3K) family. Here, we report the biologic properties of the 2-aminothiazole derivative NVP-BYL719, a selective inhibitor of PI3Kα and its most common oncogenic mutant forms. The compound selectivity combined with excellent drug-like properties translates to dose- and time-dependent inhibition of PI3Kα signaling in vivo, resulting in robust therapeutic efficacy and tolerability in PIK3CA-dependent tumors. Novel targeted therapeutics such as NVP-BYL719, designed to modulate aberrant functions elicited by cancer-specific genetic alterations upon which the disease depends, require well-defined patient stratification strategies in order to maximize their therapeutic impact and benefit for the patients. Here, we also describe the application of the Cancer Cell Line Encyclopedia as a preclinical platform to refine the patient stratification strategy for NVP-BYL719 and found that PIK3CA mutation was the foremost positive predictor of sensitivity while revealing additional positive and negative associations such as PIK3CA amplification and PTEN mutation, respectively. These patient selection determinants are being assayed in the ongoing NVP-BYL719 clinical trials. Mol Cancer Ther; 13(5); 1117–29. ©2014 AACR.

Published
2014

56. Properties of the human long and short isoforms of the uncoupling protein-3 expressed in yeast cells

Author

W. Hinz, S. Grüninger, A. De Pover, and Michele Chiesi

Subjects
Gene isoform, Succinic Acid, Biophysics, Heterologous, Saccharomyces cerevisiae, Calorimetry, Biology, Mitochondrion, Guanosine Diphosphate, Biochemistry, Ion Channels, Mitochondrial Proteins, Oxygen Consumption, Structural Biology, Uncoupling protein, Genetics, medicine, Humans, Protein Isoforms, Uncoupling Protein 3, Inner membrane, RNA, Messenger, Promoter Regions, Genetic, Molecular Biology, Uncoupling Protein 1, UCP3, Respiration, Galactose, Membrane Proteins, Skeletal muscle, Thermogenesis, Cell Biology, Malonates, Yeast, Mitochondria, medicine.anatomical_structure, Carrier Proteins
Abstract

Two splice variants of the human uncoupling protein-3 (UCP3L and UCP3S) are highly expressed in skeletal muscle. The properties of UCP3L and S have been compared to those of UCP1 in a heterologous yeast expression system under the control of the galactose promoter. Both UCP3 isoforms were found to strongly impair the coupling efficiency of respiring cells thus resulting in increased thermogenesis. The uncoupling properties of both UCP3L and S could be clearly demonstrated also in isolated yeast mitochondria both in terms of coupled respiration and in the capacity to polarize the inner membrane in conditions of limited substrate availability. Contrary to what was observed with mitochondria containing UCP1, millimolar GDP and ATP had little if any effect on the uncoupling activity of UCP3. A very marked uncoupling of whole cells and isolated mitochondria was observed at very low expression levels of UCP3S indicating that the short isoform is more active than the long one.

Published
1999
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59. The development and psychometrical evaluation of a set of instruments to evaluate the effectiveness of diabetes patient education

Author

Veerle Duprez, Marc De Spiegelaere, Dimitri Beeckman, and Marleen De Pover

Subjects
Male, medicine.medical_specialty, Psychometrics, business.industry, media_common.quotation_subject, General Medicine, Benchmarking, Systematic review, Patient satisfaction, Patient Education as Topic, Family medicine, Content validity, Diabetes Mellitus, Medicine, Humans, Quality (business), Female, business, computer, General Nursing, Delphi, Reliability (statistics), computer.programming_language, media_common
Abstract

Aims and objectives To develop a set of psychometrically sound instruments to assess knowledge, self-management and self-efficacy of diabetic patients. Furthermore, a survey to evaluate the satisfaction about diabetes education for patients was developed and tested. Background Treatment and secondary prevention of diabetes require a complex combination of care components. Patients' education has been accepted to improve diabetes knowledge, self-management and self-efficacy. Psychometrically sound instruments are needed to measure these patient-centred outcomes. Design Psychometric instrument validation. Methods The first phase included a systematic literature review to develop the instruments. Content validity was evaluated using a two-round Delphi procedure involving diabetes experts. The content validity of the instruments was excellent. In a second phase, a convenience sample of 188 diabetic patients in two hospitals in one specific care region in Belgium participated in the psychometric evaluation. The criterion-related validity and internal consistency reliability were evaluated. Results The study produced a 21-item knowledge instrument, reflecting knowledge about ‘glycemic control’ and ‘medico-social management aspects’. The self-management instrument included 32 statements, reflecting ‘treatment and compliance’ and ‘general lifestyle’. The self-efficacy instrument included 30 items, reflecting ‘nutrition’, ‘treatment’ and ‘regimen’. The patient satisfaction survey included 36 items, reflecting satisfaction about the relationship among the diabetes specialist, the diabetes educator, podiatrist and dietician. Conclusions An instrument set with sound psychometric characteristics was developed to assess knowledge, self-management and self-efficacy of diabetic patients. Future studies should focus on the association between the instrument outcomes and clinical patient outcomes. Relevance to clinical practice The current instrument can support the design of educational interventions and training programmes and reduce inconsistencies in the information that patients receive. Furthermore, the instruments can be used for benchmarking the quality of diabetic patient education.

Published
2012

60. Modulation of activation-loop phosphorylation by JAK inhibitors is binding mode dependent

Author

Debora Bonenfant, Hans Voshol, Thomas Radimerski, Catherine H. Régnier, Carole Pissot-Soldermann, Francesco Hofmann, Alain De Pover, Eric Vangrevelinghe, Zhiyan Qian, Aviva Goel, Clemens Scheufler, Fanny Marque, Hugues Ryckelynck, Priya Koppikar, Paul W. Manley, Christoph Gaul, Lorenza Wyder, Rita Andraos, Fabienne Baffert, Joëlle Rubert, William R. Sellers, Ross L. Levine, Neha Bhagwat, and Gisele A. Tavares

Subjects
Binding Sites, Kinase, Hyperphosphorylation, Plasma protein binding, Biology, Janus Kinase 2, Molecular biology, Article, Cell biology, Protein Structure, Tertiary, Mice, Protein structure, Oncology, Protein kinase domain, Cell Line, Tumor, STAT5 Transcription Factor, Phosphorylation, Animals, Humans, Binding site, Janus kinase, Protein Kinase Inhibitors, Janus Kinases, Protein Binding
Abstract

Janus kinase (JAK) inhibitors are being developed for the treatment of rheumatoid arthritis, psoriasis, myeloproliferative neoplasms, and leukemias. Most of these drugs target the ATP-binding pocket and stabilize the active conformation of the JAK kinases. This type I binding mode can lead to an increase in JAK activation loop phosphorylation, despite blockade of kinase function. Here we report that stabilizing the inactive state via type II inhibition acts in the opposite manner, leading to a loss of activation loop phosphorylation. We used X-ray crystallography to corroborate the binding mode and report for the first time the crystal structure of the JAK2 kinase domain in an inactive conformation. Importantly, JAK inhibitor–induced activation loop phosphorylation requires receptor interaction, as well as intact kinase and pseudokinase domains. Hence, depending on the respective conformation stabilized by a JAK inhibitor, hyperphosphorylation of the activation loop may or may not be elicited. Significance: This study shows that JAK inhibitors can lead to an increase of activation loop phosphorylation in a manner that is binding mode dependent. Our results highlight the need for detailed understanding of inhibitor mechanism of action, and that it may be possible to devise strategies that avoid target priming using alternative modes of inhibiting JAK kinase activity for the treatment of JAK-dependent diseases. Cancer Discov; 2(6); 512–23. © 2012 AACR. This article is highlighted in the In This Issue feature, p. 473

Published
2012

61. The central valine concept provides an entry in a new class of non peptide inhibitors of the p53-MDM2 interaction

Author

Joanna Lisztwan, Thérèse Valat, Alain De Pover, Pascal Furet, Keiichi Masuya, Joerg Kallen, and Patrick Chène

Subjects
Indole test, Models, Molecular, biology, Stereochemistry, Chemistry, Organic Chemistry, Clinical Biochemistry, Regulator, Pharmaceutical Science, Proto-Oncogene Proteins c-mdm2, Valine, Ligand (biochemistry), Biochemistry, Non peptide, P53 mdm2, Drug Discovery, biology.protein, Molecular Medicine, Mdm2, Tumor Suppressor Protein p53, Molecular Biology, P53 binding, Protein Binding
Abstract

Disrupting the interaction between the p53 tumor suppressor and its regulator MDM2 is a promising therapeutic strategy in anticancer drug research. In our search for non peptide inhibitors of this protein–protein interaction, we have devised a ligand design concept exploiting the central position of Val 93 in the p53 binding pocket of MDM2. The design of molecules based on this concept has allowed us to rapidly identify compounds having a 3-imidazolyl indole core structure as the first representatives of a new class of potent inhibitors of the p53–MDM2 interaction.

Published
2012

62. Genetic resistance to JAK2 enzymatic inhibitors is overcome by HSP90 inhibition

Author

Vincent Romanet, Bjoern Chapuy, Michael R. McKeown, David M. Weinstock, Angela V. Toms, Alain De Pover, Dirk Erdmann, Francesco Hofmann, Ross L. Levine, Oliver Weigert, Diederik van Bodegom, Liat Bird, Stephen E. Sallan, Eric Vangrevelinghe, Andrew L. Kung, Michael J. Eck, Sachie Marubayashi, Ralph Tiedt, Amanda L. Christie, Emeline Evrot, Catherine H. Régnier, Nadja Kopp, Ronald M. Paranal, James E. Bradner, Andrew A. Lane, Masato Murakami, Thomas Radimerski, Christoph Gaul, Nicolas Ebel, Akinori Yoda, and Fabienne Baffert

Subjects
Mice, 0302 clinical medicine, hemic and lymphatic diseases, polycyclic compounds, Immunology and Allergy, Phosphorylation, RNA, Small Interfering, Hsp90 Inhibitor AUY922, Luciferases, STAT5, 0303 health sciences, Mice, Inbred BALB C, Janus kinase 2, biology, food and beverages, hemic and immune systems, Flow Cytometry, Hsp90, Immunohistochemistry, 3. Good health, 030220 oncology & carcinogenesis, Female, Signal transduction, Cytokine receptor, hormones, hormone substitutes, and hormone antagonists, Signal Transduction, Immunology, Immunoblotting, Mutation, Missense, Article, 03 medical and health sciences, Heat shock protein, Cell Line, Tumor, Leukemia, B-Cell, Animals, Humans, HSP90 Heat-Shock Proteins, Receptors, Cytokine, Protein kinase B, 030304 developmental biology, Cell Proliferation, DNA Primers, Myeloproliferative Disorders, Gene Expression Profiling, Isoxazoles, Resorcinols, X-Ray Microtomography, Janus Kinase 2, Molecular biology, Mutagenesis, Cancer research, biology.protein
Abstract

Hsp90 inhibition in B cell acute lymphoblastic leukemia overcomes resistance to JAK2 inhibitors., Enzymatic inhibitors of Janus kinase 2 (JAK2) are in clinical development for the treatment of myeloproliferative neoplasms (MPNs), B cell acute lymphoblastic leukemia (B-ALL) with rearrangements of the cytokine receptor subunit cytokine receptor–like factor 2 (CRLF2), and other tumors with constitutive JAK2 signaling. In this study, we identify G935R, Y931C, and E864K mutations within the JAK2 kinase domain that confer resistance across a panel of JAK inhibitors, whether present in cis with JAK2 V617F (observed in MPNs) or JAK2 R683G (observed in B-ALL). G935R, Y931C, and E864K do not reduce the sensitivity of JAK2-dependent cells to inhibitors of heat shock protein 90 (HSP90), which promote the degradation of both wild-type and mutant JAK2. HSP90 inhibitors were 100–1,000-fold more potent against CRLF2-rearranged B-ALL cells, which correlated with JAK2 degradation and more extensive blockade of JAK2/STAT5, MAP kinase, and AKT signaling. In addition, the HSP90 inhibitor AUY922 prolonged survival of mice xenografted with primary human CRLF2-rearranged B-ALL further than an enzymatic JAK2 inhibitor. Thus, HSP90 is a promising therapeutic target in JAK2-driven cancers, including those with genetic resistance to JAK enzymatic inhibitors.

Published
2012

63. Characterisation of Na/K-ATPase, its isoforms, and the inotropic response to ouabain in isolated failing human hearts

Author

Ingrid L. Grupp, David Melvin, Alain De Pover, Jerry B. Lingrel, G. Grupp, Walter Kremers, Nathalie Gradoux, and Olga I. Shamraj

Subjects
Inotrope, medicine.medical_specialty, Digoxin, Physiology, ATPase, Ouabain, Contractility, Physiology (medical), Internal medicine, Myosin, medicine, Humans, Vanadate, RNA, Messenger, Na+/K+-ATPase, biology, Chemistry, Myocardium, Blotting, Northern, Myocardial Contraction, Stimulation, Chemical, Isoenzymes, Endocrinology, biology.protein, Sodium-Potassium-Exchanging ATPase, Cardiomyopathies, Cardiology and Cardiovascular Medicine, medicine.drug
Abstract

Objective: The aim was to determine whether failing human hearts have increased sensitivity to the inotropic and toxic effects of ouabain, and to examine alterations in Na/K-ATPase that might explain the observed higher ouabain sensitivity. Methods: For contractility studies, a total of 57 trabeculae were isolated from two non- failing (death from head injury) and 10 terminally failing, explanted human hearts. After the experiment, each trabecula was inspected under the light microscope for morphological alterations consistent with heart failure. Samples for biochemical and molecular studies were obtained from five non-failing and 13 failing hearts. Total Na/K-ATPase was measured in desoxycholate treated homogenates and expressed per unit of tissue wet or dry weight, DNA, protein, or myosin. Interference from residual bound digoxin due to previous therapy was excluded. The expression of the three α isoforms was studied at both the mRNA level using northern blots and the protein level by analysis of dissociation kinetics of the [3H]ouabain-enzyme complex. Results: Trabeculae showing morphological alterations and decreased contractility were sensitive to lower concentrations of ouabain (3-100 nM) than control trabeculae (100-1000 nM); the inotropic EC50 and the minimum toxic concentration were both reduced. [3H]Ouabain binding was significantly lower (p≪0.001) in failing than in non-failing hearts, at 293(SD 74) v 507(48) pmol·g−1 wet weight. No significant change was observed in maximum ATPase turnover rate, or in sensitivities to Na+, K+, vanadate, and dihydro-ouabain. All three α isoforms were expressed at the mRNA level in both normal and failing hearts. Conclusions: This study shows conclusively, for the first time, that failing human hearts are more sensitive to ouabain. This may be at least partly due to a mean reduction of 42% (95% confidence interval, 26 to 56%) in the concentration of Na/K-ATPase (decrease in Na,K pump reserve), but not to an alteration in its catalytic properties or in its isoform composition. Cardiovascular Research 1993; 27 :2229-2237

Published
1993
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64. Potent and selective inhibition of polycythemia by the quinoxaline JAK2 inhibitor NVP-BSK805

Author

Francesca Blasco, Eric Vangrevelinghe, Stephan Ruetz, Marc Lang, Lynda Nolan, Josef Brueggen, Markus Wartmann, Peter Drueckes, Thomas Radimerski, Lorenza Wyder, Alain De Pover, Marc Gerspacher, Gisele A. Tavares, Francesco Hofmann, Joerg Trappe, Patrick Chène, Catherine H. Régnier, Fabienne Baffert, Pascal Furet, Dirk Erdmann, David Ledieu, and Carole Pissot-Soldermann

Subjects
Models, Molecular, Cancer Research, Apoptosis, Mice, SCID, Polycythemia, Biology, Cell Line, Mice, Polycythemia vera, Adenosine Triphosphate, In vivo, hemic and lymphatic diseases, Cell Line, Tumor, Quinoxalines, medicine, STAT5 Transcription Factor, Animals, Humans, Erythropoiesis, Phosphorylation, Myelofibrosis, STAT5, Cell Proliferation, Mice, Inbred BALB C, Molecular Structure, Essential thrombocythemia, Cell growth, Kinase, Janus Kinase 2, medicine.disease, Protein Structure, Tertiary, Rats, Oncology, Biochemistry, Cell culture, Mutation, Splenomegaly, Cancer research, biology.protein, K562 Cells
Abstract

The recent discovery of an acquired activating point mutation in JAK2, substituting valine at amino acid position 617 for phenylalanine, has greatly improved our understanding of the molecular mechanism underlying chronic myeloproliferative neoplasms. Strikingly, the JAK2V617F mutation is found in nearly all patients suffering from polycythemia vera and in roughly every second patient suffering from essential thrombocythemia and primary myelofibrosis. Thus, JAK2 represents a promising target for the treatment of myeloproliferative neoplasms and considerable efforts are ongoing to discover and develop inhibitors of the kinase. Here, we report potent inhibition of JAK2V617F and JAK2 wild-type enzymes by a novel substituted quinoxaline, NVP-BSK805, which acts in an ATP-competitive manner. Within the JAK family, NVP-BSK805 displays more than 20-fold selectivity towards JAK2 in vitro, as well as excellent selectivity in broader kinase profiling. The compound blunts constitutive STAT5 phosphorylation in JAK2V617F-bearing cells, with concomitant suppression of cell proliferation and induction of apoptosis. In vivo, NVP-BSK805 exhibited good oral bioavailability and a long half-life. The inhibitor was efficacious in suppressing leukemic cell spreading and splenomegaly in a Ba/F3 JAK2V617F cell-driven mouse mechanistic model. Furthermore, NVP-BSK805 potently suppressed recombinant human erythropoietin-induced polycythemia and extramedullary erythropoiesis in mice and rats. Mol Cancer Ther; 9(7); 1945–55. ©2010 AACR.

Published
2010

65. Simultaneous protein expression and modification: an efficient approach for production of unphosphorylated and biotinylated receptor tyrosine kinases by triple infection in the baculovirus expression system

Author

Dirk, Erdmann, Catherine, Zimmermann, Patrizia, Fontana, Jean-Christophe, Hau, Alain, De Pover, and Patrick, Chène

Subjects
Cell Extracts, Staining and Labeling, Blotting, Western, Mass Spectrometry, Receptor, Insulin, Communications, Protein Structure, Tertiary, Receptor, IGF Type 1, Animals, Humans, Biotinylation, Electrophoresis, Polyacrylamide Gel, Phosphorylation, Baculoviridae, Molecular Biology, Protein Processing, Post-Translational, Chromatography, High Pressure Liquid
Abstract

Protein kinases can adopt multiple protein conformations depending on their activation status. Recently, in drug discovery, a paradigm shift has been initiated, moving from inhibition of fully activated, phosphorylated kinases to targeting the inactive, unphosphorylated forms. For identification and characterization of putative inhibitors, also interacting with the latent kinase conformation outside of the kinase domain, highly purified and homogeneous protein preparations of unphosphorylated kinases are essential. The kinetic parameters of nonphosphorylated kinases cannot be assessed easily by standard kinase enzyme assays as a result of their intrinsic autophosphorylation activity. Kinetic binding rate constants of inhibitor-protein interactions can be measured by biophysical means upon protein immobilization on chips. Protein immobilization can be achieved under mild conditions by binding biotinylated proteins to streptavidin-coated chips, exploiting the strong and highly specific streptavidin–biotin interaction. In the work reported here, the cytoplasmic domains of insulin receptor and insulin-like growth factor-1 receptor fused to a biotin ligase recognition sequence were coexpressed individually with the phosphatase YopH and the biotin-protein ligase BirA upon triple infection in insect cells. Tandem affinity purification yielded pure cytoplasmic kinase domains as judged by gel electrophoresis and HPLC. Liquid chromatography-mass spectrometry analysis showed the absence of any protein phosphorylation. Coexpression of BirA led to quantitative and site-specific biotinylation of the kinases, which had no influence on the catalytic activity of the kinases, as demonstrated by the identical phosphorylation pattern upon autoactivation and by enzymatic assay. This coexpression approach should be applicable to other protein kinases as well and should greatly facilitate the production of protein kinases in their phosphorylated and unphosphorylated state suitable for enzymatic and biophysical studies.

Published
2010

68. 2-Amino-aryl-7-aryl-benzoxazoles as potent, selective and orally available JAK2 inhibitors

Author

Christoph Gaul, Patrick Chène, Thomas Radimerski, Eric Vangrevelinghe, Carole Pissot-Soldermann, Alain De Pover, Marc Gerspacher, Ralf Endres, Dirk Erdmann, Fabienne Baffert, Francesco Hofmann, Jörg Trappe, Peter Drueckes, Marc Lang, Thomas Buhl, Reiner Aichholz, Catherine H. Régnier, Francesca Blasco, Philipp Holzer, and Pascal Furet

Subjects
Benzoxazoles, Stereochemistry, Aryl, Organic Chemistry, Clinical Biochemistry, food and beverages, Pharmaceutical Science, Administration, Oral, Benzoxazole, Janus Kinase 2, Biochemistry, Rats, chemistry.chemical_compound, Structure-Activity Relationship, chemistry, Drug Discovery, Molecular Medicine, Animals, Janus kinase, Molecular Biology, Protein Kinase Inhibitors
Abstract

A series of novel benzoxazole derivatives has been designed and shown to exhibit attractive JAK2 inhibitory profiles in biochemical and cellular assays, capable of delivering compounds with favorable PK properties in rats. Synthesis and structure–activity relationship data are also provided.

Published
2009

69. Identification and characterization of NVP-BEZ235, a new orally available dual phosphatidylinositol 3-kinase/mammalian target of rapamycin inhibitor with potent in vivo antitumor activity

Author

Kevin Schoemaker, Sauveur-Michel Maira, Alain De Pover, Saskia M. Brachmann, Pascal Furet, Josef Brueggen, William R. Sellers, Marjo Simonen, Patrick Chène, Doriano Fabbro, Daniela Gabriel, Frédéric Stauffer, Carlos Garcia-Echeverria, Christian Schnell, Peter Finan, Christine Fritsch, and Leon Murphy

Subjects
Cancer Research, Administration, Oral, Mice, Nude, Antineoplastic Agents, Pharmacology, Biology, Mice, Adenosine Triphosphate, In vivo, Cell Line, Tumor, Animals, Humans, Kinase activity, Protein kinase B, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Cell Proliferation, Phosphoinositide-3 Kinase Inhibitors, Dose-Response Relationship, Drug, Kinase, TOR Serine-Threonine Kinases, RPTOR, Cell Cycle, Imidazoles, Xenograft Model Antitumor Assays, Oncology, Quinolines, Glioblastoma, Protein Kinases, Proto-Oncogene Proteins c-akt, Ex vivo
Abstract

The phosphatidylinositol 3-kinase (PI3K)/Akt/mammalian target of rapamycin inhibitor (mTOR) pathway is often constitutively activated in human tumor cells, providing unique opportunities for anticancer therapeutic intervention. NVP-BEZ235 is an imidazo[4,5-c]quinoline derivative that inhibits PI3K and mTOR kinase activity by binding to the ATP-binding cleft of these enzymes. In cellular settings using human tumor cell lines, this molecule is able to effectively and specifically block the dysfunctional activation of the PI3K pathway, inducing G1 arrest. The cellular activity of NVP-BEZ235 translates well in in vivo models of human cancer. Thus, the compound was well tolerated, displayed disease stasis when administered orally, and enhanced the efficacy of other anticancer agents when used in in vivo combination studies. Ex vivo pharmacokinetic/pharmacodynamic analyses of tumor tissues showed a time-dependent correlation between compound concentration and PI3K/Akt pathway inhibition. Collectively, the preclinical data show that NVP-BEZ235 is a potent dual PI3K/mTOR modulator with favorable pharmaceutical properties. NVP-BEZ235 is currently in phase I clinical trials. [Mol Cancer Ther 2008;7(7):1–13 [Mol Cancer Ther 2008;7(7):1851–13]

Published
2008

72. Diabetespatiënt en fit en actief!

Author

De Wilde, W., Deforche, Benedicte, De Pover, M., Calders, P., and Biometrie en Biomechanica

Subjects
Diabetespatiënt en fit en actief!
Abstract

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Published
2005

74. Characterization of the Novel and Specific PI3Kα Inhibitor NVP-BYL719 and Development of the Patient Stratification Strategy for Clinical Trials

Author

Fritsch, Christine, primary, Huang, Alan, additional, Chatenay-Rivauday, Christian, additional, Schnell, Christian, additional, Reddy, Anupama, additional, Liu, Manway, additional, Kauffmann, Audrey, additional, Guthy, Daniel, additional, Erdmann, Dirk, additional, De Pover, Alain, additional, Furet, Pascal, additional, Gao, Hui, additional, Ferretti, Stephane, additional, Wang, Youzhen, additional, Trappe, Joerg, additional, Brachmann, Saskia M., additional, Maira, Sauveur-Michel, additional, Wilson, Christopher, additional, Boehm, Markus, additional, Garcia-Echeverria, Carlos, additional, Chene, Patrick, additional, Wiesmann, Marion, additional, Cozens, Robert, additional, Lehar, Joseph, additional, Schlegel, Robert, additional, Caravatti, Giorgio, additional, Hofmann, Francesco, additional, and Sellers, William R., additional

Published
2014
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75. Obstacles à l’application de la Valorisation des Rôles Sociaux: regard de travailleurs sociaux

Author

De Pover, Martine, Negro, Enzo, De Pover, Martine, and Negro, Enzo

Abstract

La Valorisation des Rôles Sociaux (VRS) est un concept clair et précis qui n’est pas pour autant simple d’application. En effet, il existe un écart entre ce que disent faire les professionnels (niveau expressif) et ce qu’ils font réellement (niveau effectif). C’est pourquoi, j’ai voulu identifier les obstacles que rencontrent les éducateurs, sur le plan expressif, face à l’application de la VRS ainsi que leurs ressources pour y faire face. L’analyse porte sur deux institutions différentes, qui accueillent des personnes adultes en situation de handicap. La partie théorique présente d’abord quelques notions sous-jacentes à la VRS. La suite est essentiellement basée sur le concept de la VRS (l’historique, la définition, les composantes, les moyens d’évaluation et d’auto-évaluation). A travers l’analyse, nous verrons que les principaux obstacles rencontrés par les éducateurs sont au sein de l’équipe et sur le plan personnel. Ce qui a été mis en évidence, c’est la différence de perception voir d’application de la VRS au sein de l’équipe. Sur le plan personnel, la routine et le manque de prise de recul dans l’action quotidienne sont les deux obstacles principaux relevés. L’accent n’a pas été mis sur les obstacles organisationnels. J’ai interrogé un membre de la direction par institution pour savoir quel genre d’obstacles les éducateurs rencontrent selon lui. Ainsi, le résultat m’a permis de voir qu’il y a un consensus entre les éducateurs et le membre de la direction, ceci dans les deux institutions, car mon hypothèse est infirmée moyennant quelques nuances.

Published
2013

76. Epidermal growth factor regulates fatty acid uptake and metabolism in Caco-2 cells

Author

Nathalie Gradoux, Christian Darimont, and Alain De Pover

Subjects
Saccharomyces cerevisiae Proteins, Long-chain-fatty-acid—CoA ligase, Physiology, Palmitic Acid, Biology, Fatty Acid-Binding Proteins, Myelin P2 Protein, Fatty acid-binding protein, Palmitic acid, chemistry.chemical_compound, Epidermal growth factor, Physiology (medical), Coenzyme A Ligases, Humans, Diacylglycerol O-Acyltransferase, Intestinal Mucosa, Lipid Transport, chemistry.chemical_classification, Hepatology, Epidermal Growth Factor, Tumor Suppressor Proteins, Fatty Acids, Gastroenterology, Fatty acid, Metabolism, Amino acid, Neoplasm Proteins, Intestines, Repressor Proteins, chemistry, Biochemistry, lipids (amino acids, peptides, and proteins), Caco-2 Cells, Carrier Proteins, Fatty Acid-Binding Protein 7, Acyltransferases
Abstract

Epidermal growth factor (EGF) has been reported to stimulate carbohydrate, amino acid, and electrolyte transport in the small intestine, but its effects on lipid transport are poorly documented. This study aimed to investigate EGF effects on fatty acid uptake and esterification in a human enterocyte cell line (Caco-2). EGF inhibited cell uptake of [14C]palmitate and markedly reduced its incorporation into triglycerides. In contrast, the incorporation in phospholipids was enhanced. To elucidate the mechanisms involved, key steps of lipid synthesis were investigated. The amount of intestinal fatty acid-binding protein (I-FABP), which is thought to be important for fatty acid absorption, and the activity of diacylglycerol acyltransferase (DGAT), an enzyme at the branch point of diacylglycerol utilization, were reduced. EGF effects on DGAT and on palmitate esterification occurred at 2–10 ng/ml, whereas effects on I-FABP and palmitate uptake occurred only at 10 ng/ml. This suggests that EGF inhibited palmitate uptake by reducing the I-FABP level and shifted its utilization from triglycerides to phospholipids by inhibiting DGAT. This increase in phospholipid synthesis might play a role in the restoration of enterocyte absorption function after intestinal mucosa injury.

Published
1999

77. [1] Inhibition of lipid absorption as an approach to the treatment of obesity

Author

Michael T. Clandinin, Elżbieta Jarocka-Cyrta, A. De Pover, Abr Thomson, and Monika Keelan

Subjects
Vitamin, Calorie, Fat substitute, Leptin, media_common.quotation_subject, Appetite, Lipid metabolism, medicine.disease, Obesity, chemistry.chemical_compound, chemistry, medicine, Food science, Lipid digestion, media_common
Abstract

A reduction in fat intake may be achieved by making educated choices to reduce total calorie intake, to consume a lower quantity of total fats, or to modify the ratio of saturated-to-polyunsaturated lipids. Leptin agonists or NPY or CCK antagonists may prove to be useful to diminish appetite and thereby reduce the total intake of food. But eating has such cultural, social, and hedonistic attributes that such a single-pronged approach is unlikely to be successful. The use of fat substitutes may prove to be popular to provide a wide range of snack food options, but these are likely to be of minimal use in weight reduction programs because of their distribution of additives in only a limited number of foods. The inhibitors of lipid digestion will be modestly successful in the short term; their long-term success will be influenced by gastrointestinal adverse effects and the need to consume fat-soluble vitamin supplements to prevent the development of fat-soluble vitamin deficiencies. The inhibition of lipid absorption is an attractive targeted approach for the treatment of obesity, since this would reduce the uptake of visible as well as invisible fats, which would potentially offer convenient dosing, and could also be a means to inhibit secondarily the uptake of carbohydrate calories.

Published
1997
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78. Inhibition of lipid absorption as an approach to the treatment of obesity

Author

A B, Thomson, A, De Pover, M, Keelan, E, Jarocka-Cyrta, and M T, Clandinin

Subjects
Lipoproteins, Tumor Suppressor Proteins, Satiation, Fatty Acid-Binding Proteins, Lipid Metabolism, Myelin P2 Protein, Dietary Fats, Neoplasm Proteins, Bile Acids and Salts, Intestinal Absorption, Animals, Humans, Digestion, Nutritional Physiological Phenomena, Obesity, Carrier Proteins, Fat Substitutes, Fatty Acid-Binding Protein 7
Abstract

A reduction in fat intake may be achieved by making educated choices to reduce total calorie intake, to consume a lower quantity of total fats, or to modify the ratio of saturated-to-polyunsaturated lipids. Leptin agonists or NPY or CCK antagonists may prove to be useful to diminish appetite and thereby reduce the total intake of food. But eating has such cultural, social, and hedonistic attributes that such a single-pronged approach is unlikely to be successful. The use of fat substitutes may prove to be popular to provide a wide range of snack food options, but these are likely to be of minimal use in weight reduction programs because of their distribution of additives in only a limited number of foods. The inhibitors of lipid digestion will be modestly successful in the short term; their long-term success will be influenced by gastrointestinal adverse effects and the need to consume fat-soluble vitamin supplements to prevent the development of fat-soluble vitamin deficiencies. The inhibition of lipid absorption is an attractive targeted approach for the treatment of obesity, since this would reduce the uptake of visible as well as invisible fats, which would potentially offer convenient dosing, and could also be a means to inhibit secondarily the uptake of carbohydrate calories.

Published
1997

84. Modulation of Activation-Loop Phosphorylation by JAK Inhibitors Is Binding Mode Dependent

Author

Andraos, Rita, primary, Qian, Zhiyan, additional, Bonenfant, Débora, additional, Rubert, Joëlle, additional, Vangrevelinghe, Eric, additional, Scheufler, Clemens, additional, Marque, Fanny, additional, Régnier, Catherine H., additional, De Pover, Alain, additional, Ryckelynck, Hugues, additional, Bhagwat, Neha, additional, Koppikar, Priya, additional, Goel, Aviva, additional, Wyder, Lorenza, additional, Tavares, Gisele, additional, Baffert, Fabienne, additional, Pissot-Soldermann, Carole, additional, Manley, Paul W., additional, Gaul, Christoph, additional, Voshol, Hans, additional, Levine, Ross L., additional, Sellers, William R., additional, Hofmann, Francesco, additional, and Radimerski, Thomas, additional

Published
2012
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85. Identification and Characterization of NVP-BKM120, an Orally Available Pan-Class I PI3-Kinase Inhibitor

Author

Maira, Sauveur-Michel, primary, Pecchi, Sabina, additional, Huang, Alan, additional, Burger, Matthew, additional, Knapp, Mark, additional, Sterker, Dario, additional, Schnell, Christian, additional, Guthy, Daniel, additional, Nagel, Tobi, additional, Wiesmann, Marion, additional, Brachmann, Saskia, additional, Fritsch, Christine, additional, Dorsch, Marion, additional, Chène, Patrick, additional, Shoemaker, Kevin, additional, De Pover, Alain, additional, Menezes, Daniel, additional, Martiny-Baron, Georg, additional, Fabbro, Doriano, additional, Wilson, Christopher J., additional, Schlegel, Robert, additional, Hofmann, Francesco, additional, García-Echeverría, Carlos, additional, Sellers, William R., additional, and Voliva, Charles F., additional

Published
2012
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86. Genetic resistance to JAK2 enzymatic inhibitors is overcome by HSP90 inhibition

Author

Weigert, Oliver, primary, Lane, Andrew A., additional, Bird, Liat, additional, Kopp, Nadja, additional, Chapuy, Bjoern, additional, van Bodegom, Diederik, additional, Toms, Angela V., additional, Marubayashi, Sachie, additional, Christie, Amanda L., additional, McKeown, Michael, additional, Paranal, Ronald M., additional, Bradner, James E., additional, Yoda, Akinori, additional, Gaul, Christoph, additional, Vangrevelinghe, Eric, additional, Romanet, Vincent, additional, Murakami, Masato, additional, Tiedt, Ralph, additional, Ebel, Nicolas, additional, Evrot, Emeline, additional, De Pover, Alain, additional, Régnier, Catherine H., additional, Erdmann, Dirk, additional, Hofmann, Francesco, additional, Eck, Michael J., additional, Sallan, Stephen E., additional, Levine, Ross L., additional, Kung, Andrew L., additional, Baffert, Fabienne, additional, Radimerski, Thomas, additional, and Weinstock, David M., additional

Published
2012
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87. Genetic Resistance to JAK2 Enzymatic Inhibitors Is Overcome by HSP90 Inhibition

Author

Weigert, Oliver, primary, Lane, Andrew A., additional, Bird, Liat, additional, Kopp, Nadja, additional, Toms, Angela V, additional, Gaul, Christoph, additional, Vangrevelinghe, Eric, additional, De Pover, Alain, additional, Regnier, Catherine H., additional, Erdmann, Dirk, additional, Hofmann, Francesco, additional, Eck, Michael, additional, Kung, Andrew L., additional, Radimerski, Thomas, additional, and Weinstock, David M, additional

Published
2011
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89. Abstract 3748: NVP-BYL719, a novel PI3Kalpha selective inhibitor with all the characteristics required for clinical development as an anti-cancer agent

Author

Daniel Guthy, Francesco Hofmann, Sauveur-Michel Maira, Christian Schnell, Alain De Pover, Saskia M. Brachmann, Christine Fritsch, Christian Chatenay-Rivauday, Cornelia Quadt, Alan Huang, Giorgio Caravatti, and Markus Wartmann

Subjects
Cancer Research, Kinase, Point mutation, Cancer, Pharmacology, P110α, Biology, medicine.disease, Metastasis, Oncology, In vivo, medicine, Protein kinase B, PI3K/AKT/mTOR pathway
Abstract

Most of the current oncology drug discovery and development work has shifted towards molecularly targeted therapies. A key focus has been on identifying inhibitors against components of pathways that drive tumor cell proliferation, survival, and metastasis such as the PI3K/mTOR pathway, reported to be implicated in many human cancers through various mechanisms, such as, somatic PIK3CA missense mutations that occur at high frequency. These mutations are largely point mutations predominantly clustered within three hotspots in the helical and kinase domains of p110α: E542K, E545K and H1047R, which represent about 80% of the mutations observed, and confirmed to be oncogenic gain-of-function mutations. Based on these findings cancer-specific mutants of p110α appear to be ideal targets for drug development and p110α specific inhibitors, such as NVP-BYL719, could then have potential anti-cancer activity without causing the potential side effects that could be expected from interference with other Class I PI3K isoforms or other members of the PIKK family. NVP-BYL719 is best described as a PI3Kalpha inhibitor as in biochemical assays, it inhibits p110α as well as p110α most common somatic mutations (IC50=5 nM) much more potently than p110α and ≤ and has weak or no activity against p110α, Vps34 and mTOR and is selective against a wide range of protein kinases (> 50-fold). The potency and selectivity profile of NVP-BYL719 is confirmed at the cellular level, is correlated with inhibition of various PI3K/Akt downstream signaling pathway components and is associated with anti-proliferation of breast cancer cell lines harboring PIK3CA mutations. In vivo, NVP-BYL719 shows dose and time-dependent inhibition of the PI3K/Akt pathway which correlates with compound exposure and is associated with good tolerability and significant dose-dependent anti-tumor efficacy in PIK3CA mutant tumor xenograft models in rodents. Moreover, plasma insulin levels are significantly increased while blood glucose levels remained normal at all tested doses and time points indicating on-target effects of NVP-BYL719 on the regulation of metabolism. Overall, as a PI3Kalpha inhibitor, NVP-BYL719 has good drug-like and pharmacological properties and presents all the characteristics required for its ongoing Phase I clinical development in adult patients with advanced solid malignancies whose tumors have an alteration of the PIK3CA gene. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 103rd Annual Meeting of the American Association for Cancer Research; 2012 Mar 31-Apr 4; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2012;72(8 Suppl):Abstract nr 3748. doi:1538-7445.AM2012-3748

Published
2012
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90. Abstract 1922: 2-Aminothiazoles as potent and selective PI3Kalpha inhibitors: Discovery of NVP-BYL719 and structural basis for the isoform selectivity

Author

Robin Alec Fairhurst, Mark Knapp, Giorgio Caravatti, Alain De Pover, Francesca Blasco, Frank Hans Seiler, Patricia Imbach, Doriano Fabbro, Joachim Blanz, Vito Guagnano, Christine Fritsch, Ian N. Bruce, Marc Lang, and Pascal Furet

Subjects
Gene isoform, Cancer Research, Programmed cell death, Lipid kinase activity, Cancer, Biological activity, P110α, Pharmacology, Biology, medicine.disease, Oncology, medicine, Signal transduction, PI3K/AKT/mTOR pathway
Abstract

PI3Ks are lipid kinases that control signaling pathways involved in cell proliferation, motility, cell death and cell invasion. Class I PI3K contains four isoforms, p110α, p110α, p110α and p110α which carry out non redundant signaling functions. The ≤ and ≤ isoforms are ubiquitously expressed, whereas the ≤ and ≤ isoforms are expressed primarily in lymphocytes and engaged in the regulation of immune responses. A gain of function in PI3K signaling is common to many types of human cancer, specifically mutations in PIK3CA which are found in more than 30% of various solid tumor types, including, breast, endometrium, bladder, colorectal cancers as well as lung cancers. As these mutations constitutively activate the lipid kinase activity of the protein, the cancer-specific mutants of p110α appear to be ideal therapeutic targets for anticancer drug development. p110α isoform specific low molecular weight inhibitors could be efficacious against tumors harboring p110alpha mutations and provide an improved safety profile compared to current pan-PI3K modulators. The 2-aminothiazole scaffold proved to be an excellent starting point for the development of potent PI3K inhibitors. Depending on the substitution pattern good PI3Kalpha selectivity can be achieved. Systematic modification of key residues and further optimization of the drug-like and PK properties have led to the identification of NVP-BYL719, a potent and selective PI3Kalpha inhibitor with a promising biological activity. SAR leading to the discovery of NVP-BYL719 and the structural basis for the PI3Kalpha selectivity will be discussed. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 103rd Annual Meeting of the American Association for Cancer Research; 2012 Mar 31-Apr 4; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2012;72(8 Suppl):Abstract nr 1922. doi:1538-7445.AM2012-1922

Published
2012
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91. Potent and Selective Inhibition of Polycythemia by the Quinoxaline JAK2 Inhibitor NVP-BSK805

Author

Baffert, Fabienne, primary, Régnier, Catherine H., additional, De Pover, Alain, additional, Pissot-Soldermann, Carole, additional, Tavares, Gisele A., additional, Blasco, Francesca, additional, Brueggen, Josef, additional, Chène, Patrick, additional, Drueckes, Peter, additional, Erdmann, Dirk, additional, Furet, Pascal, additional, Gerspacher, Marc, additional, Lang, Marc, additional, Ledieu, David, additional, Nolan, Lynda, additional, Ruetz, Stephan, additional, Trappe, Joerg, additional, Vangrevelinghe, Eric, additional, Wartmann, Markus, additional, Wyder, Lorenza, additional, Hofmann, Francesco, additional, and Radimerski, Thomas, additional

Published
2010
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92. Genetic Resistance to JAK2 Enzymatic Inhibitors Is Overcome by HSP90 Inhibition

Author

Eric Vangrevelinghe, Andrew L. Kung, Alain De Pover, Oliver Weigert, Catherine H. Régnier, Andrew A. Lane, Francesco Hofmann, David M. Weinstock, Michael J. Eck, Thomas Radimerski, Christoph Gaul, Angela V. Toms, Dirk Erdmann, Liat Bird, and Nadja Kopp

Subjects
Mutation, education.field_of_study, Janus kinase 2, ABL, biology, Immunology, Mutant, Population, food and beverages, Cell Biology, Hematology, TG101348, medicine.disease_cause, Resistance mutation, Biochemistry, Molecular biology, chemistry.chemical_compound, chemistry, hemic and lymphatic diseases, biology.protein, medicine, education, Tyrosine kinase
Abstract

Abstract 62 Mutation within the kinase domain of tyrosine kinases is a common mechanisms of resistance to enzymatic inhibitors. Inhibitors of janus kinase 2 (JAK2) are under evaluation in patients with myeloproliferative neoplasms (MPNs), B-cell acute lymphoblastic leukemia (B-ALL) with rearrangements of the cytokine receptor subunit CRLF2, and other tumors with constitutive JAK2 signaling. To identify resistance mutations in JAK2, we randomly mutagenized human JAK2 R683G, which is observed in approximately half of CRLF2-rearranged B-ALL. We transduced the mutagenized JAK2 cDNA library into murine Ba/F3 cells that express CRLF2. Expression of CRLF2 and JAK2 R683G confers IL3 independent growth in Ba/F3 cells. The transduced population was selected in the JAK2-selective inhibitor NVP-BVB808 in the absence of IL3. Multiple BVB808-resistant clones were recovered that harbored either E864K, Y931C or G935R mutations in JAK2. Alignment of homologous regions of the JAK2 kinase domain (JH1) with ABL1 demonstrated that the three mutations are located in regions homologous to imatinib resistance hotspots in ABL1. Codons Y931 and G935 are within the hinge region of the kinase domain. Based on structural modeling, Y931C is likely to inhibit substrate binding. E864K is located in the middle of b3 following the P-loop in the N-lobe and may modify the structure and flexibility of the preceding P-loop, thus destabilizing the conformation required for inhibitor binding. We expressed JAK2 V617F alleles harboring Y931C, G935R or E864K in Ba/F3-EPOR cells and exposed the cells to the JAK2 enzymatic inhibitors JAK inhibitor-1, NVP-BSK805, TG101348, tofacitinib (formerly tasocitnib), ruxolitinib (formerly INCB18424) and BVB808. All three mutations conferred 2- to >10-fold resistance against BVB808, NVP-BSK805, TG101348, ruxolitinib and JAK inhibitor-1. Y931C and E864K but not G935R conferred resistance to tofactinib. Modeling of G935R indicated that a 935R side-chain would occlude the hydrophobic channel of the ATP-binding pocket. As a consequence, this mutation would decrease the binding affinity of compounds occupying the hydrophobic channel like JAK inhibitor-1 or BSK805, but not affect the potency of tofactinib, which does not bind in this region. Mutation of G935 to arginine, histidine or glutamine reduced the inhibitory effects of JAK inhibitor-1, but not tofacitinib, on JAK2 kinase domain activity. None of the codon 935 mutations had significant effects on Km or Vmaxin vitro. BVB808 treatment partially reduced activation state-specific phosphorylation of STAT5 in Ba/F3-EPOR/JAK2 V617F cells but not in Ba/F3-EPOR/JAK2 V617F/G935R or G935H cells. JAK2 is a known client of HSP90, and HSP90 inhibitors promote the degradation of both wild-type and mutant JAK2. We hypothesized that resistance mutations within the JAK2 kinase domain would not affect JAK2 degradation induced by HSP90 inhibitors. We assayed the cytotoxicity of the resorcinylic isoxazole amide NVP-AUY922 and the benzoquinone ansamycin 17-AAG in Ba/F3 cells that express the erythropoietin receptor (EPOR) and JAK2 V617F, which is observed in more than half of MPNs. Mutation of JAK2 V617F to include E864K, Y931C or G935R did not affect sensitivity to either AUY922 or 17-AAG. In fact, AUY922 was more active against cells harboring G935R (GI50, 3.87 nM) or E864K (GI50, 6.14 nM) compared to cells with no resistance mutation (GI50, 14.7 nM; p Disclosures: Gaul: Novartis: Employment. Vangrevelinghe:Novartis: Employment. De Pover:Novartis: Employment. Regnier:Novartis: Employment. Erdmann:Novartis: Employment. Hofmann:Novartis: Employment. Eck:Novartis: Consultancy, Research Funding. Kung:Novartis Pharmaceuticals: Consultancy, Research Funding. Radimerski:Novartis Pharma AG: Employment. Weinstock:Novartis: Consultancy, Research Funding.

Published
2011
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93. Novel, Potent and Selective JAK2 Inhibitors.

Author

Radimerski, Thomas, primary, Baffert, Fabienne, additional, Regnier, Catherine H., additional, De Pover, Alain, additional, Pissot, Carole, additional, Gerspacher, Marc, additional, Brueggen, Josef, additional, Tavares, Gisele, additional, Blasco, Francesca, additional, Ledieu, David, additional, Nolan, Lynda, additional, Ruetz, Stephan, additional, Chene, Patrick, additional, Erdmann, Dirk, additional, Drueckes, Peter, additional, Furet, Pascal, additional, Lang, Marc, additional, Trappe, Joerg, additional, Vangrevelinghe, Eric, additional, Wartmann, Markus, additional, and Hofmann, Francesco, additional

Published
2009
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94. Kinetic Study of Human Full-Length Wild-Type JAK2 and V617F Mutant Proteins

Author

Erdmann, Dirk, primary, Allard, Bertrand, additional, Bohn, Jacqueline, additional, De Pover, Alain, additional, Floersheimer, Andreas, additional, Fontana, Patrizia, additional, Gerspacher, Marc, additional, Hau, Jean Christophe, additional, Hofmann, Francesco, additional, Radimerski, Thomas, additional, Wille, Roman, additional, Zimmermann, Catherine, additional, and Chene, Patrick, additional

Published
2009
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95. Identification and characterization of NVP-BEZ235, a new orally available dual phosphatidylinositol 3-kinase/mammalian target of rapamycin inhibitor with potent in vivo antitumor activity

Author

Maira, Sauveur-Michel, primary, Stauffer, Frédéric, additional, Brueggen, Josef, additional, Furet, Pascal, additional, Schnell, Christian, additional, Fritsch, Christine, additional, Brachmann, Saskia, additional, Chène, Patrick, additional, De Pover, Alain, additional, Schoemaker, Kevin, additional, Fabbro, Doriano, additional, Gabriel, Daniela, additional, Simonen, Marjo, additional, Murphy, Leon, additional, Finan, Peter, additional, Sellers, William, additional, and García-Echeverría, Carlos, additional

Published
2008
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96. Novel, Potent and Selective JAK2 Inhibitors

Author

Francesca Blasco, Fabienne Baffert, Pascal Furet, Dirk Erdmann, Alain De Pover, Thomas Radimerski, Marc Lang, Gisele A. Tavares, Eric Vangrevelinghe, Stephan Ruetz, Markus Wartmann, Josef Brueggen, Peter Drueckes, David Ledieu, Patrick Chène, Marc Gerspacher, Carole Pissot, Francesco Hofmann, Lynda Nolan, Catherine H. Régnier, and Joerg Trappe

Subjects
business.industry, Extramedullary erythropoiesis, Immunology, Rat model, Myeloproliferative disease, Cell Biology, Hematology, JAK Family, Pharmacology, Biochemistry, Molecular mechanism, Medicine, Jak2v617f mutation, business, Cell spreading
Abstract

Abstract 3777 Poster Board III-713 The recent discovery of an acquired activating point mutation in JAK2, substituting valine at amino acid position 617 for phenylalanine, has greatly improved our understanding of the molecular mechanism underlying chronic myeloproliferative neoplasms. Strikingly, the JAK2V617F mutation is found in nearly all patients suffering from polycythemia vera and in roughly every second patient suffering from essential thrombocythemia and from primary myelofibrosis. Thus, JAK2 represents a promising target for the treatment of myeloproliferative disorders and considerable efforts are ongoing to discover and develop inhibitors of the kinase. Here, we report potent inhibition of JAK2V617F and JAK2 wild type enzymes by novel small molecule inhibitors, which act in an ATP-competitive manner. The profile of a lead compound from this class will be presented that displays more than twenty-fold selectivity towards JAK2 within the JAK family, as well as excellent selectivity in broader kinase profiling. The compound blunts constitutive STAT5 phosphorylation in JAK2V617F-bearing cells, with concomitant suppression of cell proliferation and induction of apoptosis. In vivo, the inhibitor exhibited good oral bioavailability and is efficacious in suppressing leukemic cell spreading and splenomegaly in a Ba/F3 JAK2V617F cell-driven mouse mechanistic model as well as polycythemia and extramedullary erythropoiesis in mouse and rat models. Disclosures: Radimerski: Novartis: Employment, Equity Ownership. Baffert:Novartis: Employment. Regnier:Novartis: Employment. De Pover:Novartis: Employment. Pissot:Novartis: Employment. Gerspacher:Novartis: Employment. Brueggen:Novartis: Employment. Tavares:Novartis: Employment. Blasco:Novartis: Employment. Ledieu:Novartis: Employment. Nolan:Novartis: Employment. Ruetz:Novartis: Employment. Chene:Novartis: Employment. Erdmann:Novartis: Employment. Drueckes:Novartis: Employment. Furet:Novartis: Employment. Lang:Novartis: Employment. Trappe:Novartis: Employment. Vangrevelinghe:Novartis: Employment. Wartmann:Novartis: Employment. Hofmann:Novartis: Employment.

Published
2009
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98. Towards an improved health care relationship with diabetes living in poverty

Author

Bieke Crabbe, A De Craecker, M. De Pover, Guido Schoorens, Veerle Duprez, and Veerle Devriendt

Subjects
medicine.medical_specialty, Nutrition and Dietetics, Poverty, business.industry, Endocrinology, Diabetes and Metabolism, medicine.disease, Nursing, Diabetes mellitus, Family medicine, Health care, Internal Medicine, Self care, medicine, Family Practice, business, Health policy
Published
2007
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