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1. Cereblon-recruiting proteolysis targeting chimeras (PROTACs) can determine the selective degradation of HDAC1 over HDAC3.

4. Heme binding to human CLOCK affects interactions with the E-box

6. Aster-dependent nonvesicular transport facilitates dietary cholesterol uptake

11. Hydroxamic Acid-Modified Peptide Library Provides Insights into the Molecular Basis for the Substrate Selectivity of HDAC Corepressor Complexes

15. Targeting the CoREST complex with dual histone deacetylase and demethylase inhibitors

19. Histone H2B Deacylation Selectivity: Exploring Chromatin’s Dark Matter with an Engineered Sortase

20. Structure-Guided Approach to Relieving Transcriptional Repression in Resistance to Thyroid Hormone α

22. A specific mutation in TBL1XR1 causes Pierpont syndrome

23. Transient Expression in HEK 293 Cells: An Alternative to E. coli for the Production of Secreted and Intracellular Mammalian Proteins

31. A de novo substitution in BCL11B leads to loss of interaction with transcriptional complexes and craniosynostosis

33. Insights into the activation mechanism of class I HDAC complexes by inositol phosphates

35. A conserved structural motif reveals the essential transcriptional repression function of Spen proteins and their role in developmental signaling

38. The structure of the ultraspiracle ligand-binding domain reveals a nuclear receptor locked in an inactive conformation

39. Mutations in TBL1X Are Associated With Central Hypothyroidism

40. A specific mutation inTBL1XR1causes Pierpont syndrome

41. A Pharmacogenetic Approach to the Treatment of Patients With Mutations.

42. The ansamycin antibiotic, rifamycin SV, inhibits BCL6 transcriptional repression and forms a complex with the BCL6-BTB/POZ domain

44. Mzt1/Tam4, a fission yeast MOZART1 homologue, is an essential component of the gamma-tubulin complex and directly interacts with GCP3(Alp6)

46. The IDOL-UBE2D complex mediates sterol-dependent degradation of the LDL receptor.

47. FERM-dependent E3 ligase recognition is a conserved mechanism for targeted degradation of lipoprotein receptors

48. Structural basis for the assembly of the SMRT/NCoR core transcriptional repression machinery

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