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1. The homodimerization domain of the Stl repressor is crucial for efficient inhibition of mycobacterial dUTPase

2. Beyond Chelation: EDTA Tightly Binds Taq DNA Polymerase, MutT and dUTPase and Directly Inhibits dNTPase Activity

3. The Role of a Key Amino Acid Position in Species-Specific Proteinaceous dUTPase Inhibition

4. Substrate Tunnel Engineering Aided by X-ray Crystallography and Functional Dynamics Swaps the Function of MIO-Enzymes

5. Synthesis of New Chiral Crown Ethers Containing Phosphine or Secondary Phosphine Oxide Units

7. Structural insights into the tyrosine phosphorylation–mediated inhibition of SH3 domain–ligand interactions

9. Structural characterization of a sodium perchlorate−acridino-18-crown-6 ether complex

10. Beyond Chelation: EDTA Tightly Binds Taq DNA Polymerase, MutT and dUTPase and Directly Inhibits dNTPase Activity

11. Structural characterization of the crystalline diastereomeric complexes of enantiopure dimethylacridino-18-crown-6 ether and the enantiomers of 1-(1-naphthyl)ethylamine hydrogen perchlorate

12. Structural characterization of a complex derived from lead(II) perchlorate and acridono-18-crown-6 ether

13. Molecular dynamics of the cryo-EM CFTR structure

14. The First Enantioselective Total Synthesis of (-)-trans-Dihydronarciclasine

15. Highly potent dUTPase inhibition by a bacterial repressor protein reveals a novel mechanism for gene expression control

16. Structural snapshots of multiple enzyme–ligand complexes pave the road for semi-rational enzyme engineering

17. Oncogenic KRAS G12C mutation-derived inhibitor development

18. Structural Characterization of Arginine Fingers: Identification of an Arginine Finger for the Pyrophosphatase dUTPases

19. Origin of problems related to Staudinger reduction in carbopeptoid syntheses

20. Association of RNA with the uracil-DNA-degrading factor has major conformational effects and is potentially involved in protein folding

24. Direct contacts between conserved motifs of different subunits provide major contribution to active site organization in human and mycobacterial dUTPases

25. A Hidden Active Site in the Potential Drug Target Mycobacterium tuberculosis dUTPase Is Accessible through Small Amplitude Protein Conformational Changes

27. Regulation of the Equilibrium between Closed and Open Conformations of Annexin A2 by N-Terminal Phosphorylation and S100A4-Binding

28. Preventive DNA repair by sanitizing the cellular (deoxy)nucleoside triphosphate pool

29. Structure and enzymatic mechanism of a moonlighting dUTPase

30. Crystallization and preliminary crystallographic analysis of dUTPase from the φ11 helper phage of Staphylococcus aureus

31. Association of RNA with the uracil-DNA-degrading factor has major conformational effects and is potentially involved in protein folding

32. Aromatic stacking between nucleobase and enzyme promotes phosphate ester hydrolysis in dUTPase

33. A novel fruitfly protein under developmental control degrades uracil-DNA

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