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1. An acetylation-mediated chromatin switch governs H3K4 methylation read-write capability

2. Parallel functional annotation of cancer-associated missense mutations in histone methyltransferases

3. Disentangling the recognition complexity of a protein hub using a nanopore

4. Structure analysis suggests Ess1 isomerizes the carboxy-terminal domain of RNA polymerase II via a bivalent anchoring mechanism

5. EGCG binds intrinsically disordered N-terminal domain of p53 and disrupts p53-MDM2 interaction

6. High affinity binding of H3K14ac through collaboration of bromodomains 2, 4 and 5 is critical for the molecular and tumor suppressor functions of PBRM1

7. Convergent Alterations of a Protein Hub Produce Divergent Effects within a Binding Site

8. Interplay of Affinity and Surface Tethering in Protein Recognition

9. Data publication with the structural biology data grid supports live analysis

11. A histone methyltransferase point mutation demonstrates a mechanism for translocation-driven acute leukemias

12. Mechanistic insights into enhancement or inhibition of phase separation by different polyubiquitin chains

13. Structure analysis suggests Ess1 isomerizes the carboxy-terminal domain of RNA polymerase II via a bivalent anchoring mechanism

14. Multistate structures of the MLL1-WRAD complex bound to H2B-ubiquitinated nucleosome

15. An acetylation-mediated chromatin switch governs H3K4 methylation read-write capability

17. Mechanistic insights into the enhancement or inhibition of phase separation by polyubiquitin chains of different lengths or linkages

18. Probing multiple enzymatic methylation events in real time with NMR spectroscopy

19. Kinetics of the multitasking high-affinity Win binding site of WDR5 in restricted and unrestricted conditions

20. EGCG binds intrinsically disordered N-terminal domain of p53 and disrupts p53-MDM2 interaction

21. Exploring the kinetics of the Win-site of WDR5

22. Hierarchical assembly of the MLL1 core complex within a biomolecular condensate regulates H3K4 methylation

24. High affinity binding of H3K14ac through collaboration of bromodomains 2, 4 and 5 is critical for the molecular and tumor suppressor functions of PBRM1

25. Unique Role of the WD-40 Repeat Protein 5 (WDR5) Subunit within the Mixed Lineage Leukemia 3 (MLL3) Histone Methyltransferase Complex

26. Biochemical Reconstitution and Phylogenetic Comparison of Human SET1 Family Core Complexes Involved in Histone Methylation

27. Trithorax monomethylates histone H3K4 and interacts directly with CBP to promote H3K27 acetylation and antagonize Polycomb silencing

28. Automethylation Activities within the Mixed Lineage Leukemia-1 (MLL1) Core Complex Reveal Evidence Supporting a 'Two-active Site' Model for Multiple Histone H3 Lysine 4 Methylation

30. ALS-Linked Mutations Affect UBQLN2 Oligomerization and Phase Separation in a Position- and Amino Acid-Dependent Manner

32. Targeted Disruption of the Interaction between WD-40 Repeat Protein 5 (WDR5) and Mixed Lineage Leukemia (MLL)/SET1 Family Proteins Specifically Inhibits MLL1 and SETd1A Methyltransferase Complexes*

33. Protein-like Nanoparticles Based on Orthogonal Self-Assembly of Chimeric Peptides

34. Data publication with the structural biology data grid supports live analysis

35. The Bin3 RNA methyltransferase targets 7SK RNA to control transcription and translation

36. Myosin5a Tail Associates Directly with Rab3A-containing Compartments in Neurons

37. Mixed lineage leukemia: a structure-function perspective of the MLL1 protein

38. On the Mechanism of Multiple Lysine Methylation by the Human Mixed Lineage Leukemia Protein-1 (MLL1) Core Complex

39. Structure of WDR5 Bound to Mixed Lineage Leukemia Protein-1 Peptide

40. The Structural Basis of Sirtuin Substrate Affinity

41. How does the histone code work?

42. A core nucleosome surface crucial for transcriptional silencing

43. The Catalytic Mechanism of Glucose 6-Phosphate Dehydrogenases: Assignment and 1H NMR Spectroscopy pH Titration of the Catalytic Histidine Residue in the 109 kDa Leuconostoc mesenteroides Enzyme

44. Characterization of the Grp94/OS-9 chaperone-lectin complex

45. A non-active-site SET domain surface crucial for the interaction of MLL1 and the RbBP5/Ash2L heterodimer within MLL family core complexes

46. Delineation of the Roles of Amino Acids Involved in the Catalytic Functions of Leuconostoc mesenteroides Glucose 6-Phosphate Dehydrogenase

47. An Examination of the Role of Asp-177 in the His-Asp Catalytic Dyad of Leuconostoc mesenteroides Glucose 6-Phosphate Dehydrogenase: X-ray Structure and pH Dependence of Kinetic Parameters of the D177N Mutant Enzyme

48. On the Mechanism of the Reaction Catalyzed by Glucose 6-Phosphate Dehydrogenase

49. PHinDing a New Histone 'Effector' Domain

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