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1. Dual TTK/PLK1 inhibition has potent anticancer activity in TNBC as monotherapy and in combination

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

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

4. 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

5. 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

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

8. 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

9. 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

11. IL-7 Receptor Mutations and Steroid Resistance in Pediatric T cell Acute Lymphoblastic Leukemia: A Genome Sequencing Study.

12. Chemotherapy sensitivity testing on ovarian cancer cells isolated from malignant ascites

13. High-Throughput Fluorescence-Based Activity Assay for Arginase-1

14. Abstract 5646: BAL0891: A novel, small molecule, dual TTK/PLK1 mitotic checkpoint inhibitor (MCI) that drives aberrant tumor cell division

15. Abstract 5645: BAL0891: A novel dual TTK/PLK1 mitotic checkpoint inhibitor (MCI) that drives aberrant tumor cell division resulting in potent anti-cancer activity

16. LCK inhibition downregulates YAP activity and is therapeutic in patient-derived models of cholangiocarcinoma

17. Selective Targeting of CTNBB1-, KRAS- or MYC-Driven Cell Growth by Combinations of Existing Drugs.

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

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

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

21. Mapping Arginase Expression with

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

23. Abstract 1480: Comparative cancer cell panel profiling of kinase inhibitors approved for clinical use from 2018 to 2020

24. Abstract 1080: Altered response to BET-bromodomain inhibitors JQ1 and I-BET-762 targeting c-Myc in erdafitinib-resistant endometrial carcinoma cell line AN3 CA

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

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

27. Optimierte Bindungsdauer am Zielenzym: Typ-I1/2 -Inhibitoren der p38α-MAP-Kinase mit verbesserter Bindungskinetik durch direkte Interaktion mit der R-Spine

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

29. 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

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

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

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

33. Abstract 279A: Cell panel profiling of 162 small molecule therapeutics identifies response biomarkers for PARP, BET-family and proteasome inhibitors

34. Abstract 2221: Chemotherapy sensitivity of tumor cells from ascites of ovarian cancer patients: Relationship with immune status and clinical response

35. Abstract 5604: High TDO and IDO1 expression in ovarian cancer-associated cells isolated from malignant ascites

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

37. Abstract 4907: Cell line panel profiling reveals novel drug response biomarkers for BTK and CDK4/6 inhibitors

38. TTK Inhibitors as a Targeted Therapy for

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

40. 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

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

42. PO-495 Prediction of chemotherapy sensitivity on ascites of ovarian cancer patients

43. 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

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

45. Synthetic heparin derivatives as new anticoagulant drugs

47. Identification of Ligands for the Orphan Nuclear Receptor GCNF

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

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

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

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