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1. Development of allosteric and selective CDK2 inhibitors for contraception with negative cooperativity to cyclin binding

3. Stability of the Human Hsp90-p50Cdc37 Chaperone Complex against Nucleotides and Hsp90 Inhibitors, and the Influence of Phosphorylation by Casein Kinase 2

4. Ack1 mediated AKT/PKB tyrosine 176 phosphorylation regulates its activation.

5. Screening through Lead Optimization of High Affinity, Allosteric Cyclin-Dependent Kinase 2 (CDK2) Inhibitors as Male Contraceptives That Reduce Sperm Counts in Mice

7. Bivalent BET Bromodomain Inhibitors Confer Increased Potency and Selectivity for BRDT via Protein Conformational Plasticity

8. Supplementary Data from EP300 Selectively Controls the Enhancer Landscape of MYCN-Amplified Neuroblastoma

9. Data from EP300 Selectively Controls the Enhancer Landscape of MYCN-Amplified Neuroblastoma

10. Supplementary Tables S1-S3 and Figures S1-S11 from Potent Dual BET Bromodomain-Kinase Inhibitors as Value-Added Multitargeted Chemical Probes and Cancer Therapeutics

11. Data from Potent Dual BET Bromodomain-Kinase Inhibitors as Value-Added Multitargeted Chemical Probes and Cancer Therapeutics

12. Supplementary Tables S4, S5 from Potent Dual BET Bromodomain-Kinase Inhibitors as Value-Added Multitargeted Chemical Probes and Cancer Therapeutics

13. Supplementary Figure 2 from RKI-1447 Is a Potent Inhibitor of the Rho-Associated ROCK Kinases with Anti-Invasive and Antitumor Activities in Breast Cancer

14. Supplementary Table 2 from RKI-1447 Is a Potent Inhibitor of the Rho-Associated ROCK Kinases with Anti-Invasive and Antitumor Activities in Breast Cancer

15. Supplementary Table 4 from RKI-1447 Is a Potent Inhibitor of the Rho-Associated ROCK Kinases with Anti-Invasive and Antitumor Activities in Breast Cancer

16. Supplementary Table 3 from RKI-1447 Is a Potent Inhibitor of the Rho-Associated ROCK Kinases with Anti-Invasive and Antitumor Activities in Breast Cancer

17. Supplementary Figure 4 from RKI-1447 Is a Potent Inhibitor of the Rho-Associated ROCK Kinases with Anti-Invasive and Antitumor Activities in Breast Cancer

18. Supplementary Figure 1 from RKI-1447 Is a Potent Inhibitor of the Rho-Associated ROCK Kinases with Anti-Invasive and Antitumor Activities in Breast Cancer

19. Supplementary Table 1 from RKI-1447 Is a Potent Inhibitor of the Rho-Associated ROCK Kinases with Anti-Invasive and Antitumor Activities in Breast Cancer

20. Data from RKI-1447 Is a Potent Inhibitor of the Rho-Associated ROCK Kinases with Anti-Invasive and Antitumor Activities in Breast Cancer

21. Supplementary Figure 3 from RKI-1447 Is a Potent Inhibitor of the Rho-Associated ROCK Kinases with Anti-Invasive and Antitumor Activities in Breast Cancer

22. New Design Rules for Developing Potent Cell-Active Inhibitors of the Nucleosome Remodeling Factor (NURF) via BPTF Bromodomain Inhibition

23. Development of Dimethylisoxazole-Attached Imidazo[1,2-a]pyridines as Potent and Selective CBP/P300 Inhibitors

24. The discovery of high affinity and metabolically stable allosteric cyclin-dependent kinase 2 (CDK2) inhibitors from screening through lead optimization

25. 1,4-Dihydropyridinebutyrolactone-derived ring-opened ester and amide analogs targeting BET bromodomains

26. Development of allosteric, selective cyclin-dependent kinase 2 (CDK2) inhibitors that are negatively cooperative with cyclin binding and show potential as contraceptive agents

27. Structural Insights into JAK2 Inhibition by Ruxolitinib, Fedratinib, and Derivatives Thereof

28. Inhibition of p53 DNA binding by a small molecule protects mice from radiation toxicity

29. Abstract 3839: Discovery of GSTZ1 as a novel target for drug refractory non-small cell lung cancer by using fragment-based chemical proteomics

30. Dihydropyridine Lactam Analogs Targeting BET Bromodomains

31. Synthesis and Structural Characterization of a Monocarboxylic Inhibitor for GRB2 SH2 Domain

32. Structural Basis of Inhibitor Selectivity in the BRD7/9 Subfamily of Bromodomains

33. New inhibitors for the BPTF bromodomain enabled by structural biology and biophysical assay development

34. Identification and Screening of Selective WEE2 Inhibitors to Develop Non‐Hormonal Contraceptives that Specifically Target Meiosis

35. Tumor-derived CK1α mutations enhance MDMX inhibition of p53

36. Development of Dimethylisoxazole-Attached Imidazo[1,2

37. EP300 Selectively Controls the Enhancer Landscape of MYCN-Amplified Neuroblastoma

38. Group 3 medulloblastoma transcriptional networks collapse under domain specific EP300/CBP inhibition

39. Tetrahydroindazole inhibitors of CDK2/cyclin complexes

40. <scp>MDMX</scp> inhibits casein kinase 1α activity and stimulates Wnt signaling

41. Development of WEE2 kinase inhibitors as novel non-hormonal female contraceptives that target meiosis†

42. Targeting the BRD4-HOXB13 Coregulated Transcriptional Networks with Bromodomain-Kinase Inhibitors to Suppress Metastatic Castration-Resistant Prostate Cancer

43. Ligand-mediated protein degradation reveals functional conservation among sequence variants of the CUL4-type E3 ligase substrate receptor cereblon

44. Structural Basis of ALDH1A2 Inhibition by Irreversible and Reversible Small Molecule Inhibitors

45. Structure–Activity Studies of N‐Butyl‐1‐deoxynojirimycin (NB‐DNJ) Analogues: Discovery of Potent and Selective Aminocyclopentitol Inhibitors of GBA1 and GBA2

46. Structural Basis of Wee Kinases Functionality and Inactivation by Diverse Small Molecule Inhibitors

47. Advances of small molecule targeting of kinases

48. Identification of a Novel Class of BRD4 Inhibitors by Computational Screening and Binding Simulations

49. Ligand-induced global conformational changes in TBP-associated factor 1 (TAF1) tandem bromodomains – a novel strategy for targeting the TAF1

50. Abstract 2318: EP300 selectively controls the enhancer landscape of high risk neuroblastoma

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