22 results on '"Egawa D"'
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2. Crystal structure of CERT START domain in complex with compound E16
3. Crystal structure of CERT START domain in complex with compound B5
4. Crystal structure of CERT START domain in complex with compound SC1
5. Crystal structure of CERT START domain in complex with compound D16
6. Interaction between vitamin D receptor and coactivator peptide SRC2-3
7. Crystal structure of hPPARgamma ligand binding domain complexed with 17-oxoDHA
8. Ternary complex of hPPARalpha ligand binding domain, 17-oxoDHA and a SRC1 peptide
9. hPPARgamma Ligand binding domain in complex with 6-oxo-tetracosahexaenoic acid
10. hPPARgamma Ligand binding domain in complex with 5-oxo-tricosahexaenoic acid
11. Research of acupuncuture point(Houhai) in bovine on the index value of reproductive efficiency and puncture method.
12. α-Pyrrolidinononanophenone derivatives induce differentiated SH-SY5Y neuroblastoma cell apoptosis via reduction of antioxidant capacity: Involvement of NO depletion and inactivation of Nrf2/HO1 signaling pathway.
13. Covalent Modifier Discovery Using Hydrogen/Deuterium Exchange-Mass Spectrometry.
14. Involvement of a Cluster of Basic Amino Acids in Phosphorylation-Dependent Functional Repression of the Ceramide Transport Protein CERT.
15. Structural Insights into the Loss-of-Function R288H Mutant of Human PPARγ.
16. Phosphoinositide binding by the PH domain in ceramide transfer protein (CERT) is inhibited by hyperphosphorylation of an adjacent serine-repeat motif.
17. SRC2-3 binds to vitamin D receptor with high sensitivity and strong affinity.
18. 17-OxoDHA Is a PPARα/γ Dual Covalent Modifier and Agonist.
19. Apo- and Antagonist-Binding Structures of Vitamin D Receptor Ligand-Binding Domain Revealed by Hybrid Approach Combining Small-Angle X-ray Scattering and Molecular Dynamics.
20. Helix12-Stabilization Antagonist of Vitamin D Receptor.
21. Characterization of covalent bond formation between PPARγ and oxo-fatty acids.
22. A mixed population of antagonist and agonist binding conformers in a single crystal explains partial agonism against vitamin D receptor: active vitamin D analogues with 22R-alkyl group.
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