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8. NMR and molecular recognition: The interaction of human galectin-4 with the histo blood group antigens and with pathogen-associated molecules

9. Probing altered receptor specificities of antigenically drifting human H3N2 viruses by chemoenzymatic synthesis, NMR, and modeling

10. Insights into the recognition of hypermucoviscous Klebsiella pneumoniae clinical isolates by innate immune lectins of the Siglec and galectin families.

12. Correction to “Targeting the Spike: Repurposing Mithramycin and Dihydroergotamine to Block SARS-CoV-2 Infection”

14. Molecular Recognition of Glycan-Bearing Glycomacromolecules Presented at Membrane Surfaces by Lectins: An NMR View

15. Molecular Recognition of Glycan-Bearing Glycomacromolecules Presented at Membrane Surfaces by Lectins: An NMR View

16. Exploring multivalent carbohydrate–protein interactions by NMR

17. Discovery of processive catalysis by an exo-hydrolase with a pocket-shaped active site

18. Immobilization of Biantennary N-Glycans Leads to Branch Specific Epitope Recognition by LSECtin

20. Galectin-4 N-terminal domain: binding preferences toward A and B antigens with different peripheral core presentations

21. Recent advances in the application of NMR methodologies to analyze the conformation, dynamics, and interactions of saccharides

22. Molecular recognition in C‐type lectins: the cases of DC‐SIGN, Langerin, MGL, and L‐sectin

23. The SARS-CoV-2 Spike Glycoprotein Directly Binds Exogeneous Sialic Acids: A NMR View

24. Proceedings of workshop: “Neuroglycoproteins in health and disease”, INNOGLY cost action

25. Proceedings of workshop: “Neuroglycoproteins in health and disease”, INNOGLY cost action

26. Assessing the Mobility of Severe Acute Respiratory Syndrome Coronavirus-2 Spike Protein Glycans by Structural and Computational Methods

28. Minimizing the entropy penalty for ligand binding: lessons from the molecular recognition of the histo blood-group antigens by human galectin-3

30. Synthesis and chelation study of a fluoroionophore and a glycopeptide based on an aza crown iminosugar structure

31. Cross-Linking Effects Dictate the Preference of Galectins to Bind LacNAc-Decorated HPMA Copolymers

32. Selective C-13-Labels on Repeating Glycan Oligomers to Reveal Protein Binding Epitopes through NMR: Polylactosamine Binding to Galectins

33. Glycosyl Oxocarbenium Ions: Structure, Conformation, Reactivity, and Interactions

34. Galectin-4 N-Terminal Domain: Binding Preferences Toward A and B Antigens with Different Peripheral Core Presentations

35. The two domains of human galectin-8 bind sialyl- and fucose-containing oligosaccharides in an independent manner. A 3D view by using NMR

36. Kinetic Studies of Acetyl Group Migration between the Saccharide Units in an Oligomannoside Trisaccharide Model Compound and a Native Galactoglucomannan Polysaccharide

37. Exploration of galectin ligands displayed on gram-negative respiratory bacterial pathogens with different cell surface architectures

40. Unravelling the Time Scale of Conformational Plasticity and Allostery in Glycan Recognition by Human Galectin-1

41. Molecular Recognition in C-Type Lectins: The Cases of DC- SIGN, Langerin, MGL, and L-Sectin

42. Structure of a protective epitope reveals the importance of acetylation of Neisseria meningitidis serogroup A capsular polysaccharide

43. Structural Characterization of N-Linked Glycans in the Receptor Binding Domain of the SARS-CoV-2 Spike Protein and their Interactions with Human Lectins

44. Mono and Di-Fucosylated Glycans of the Parasitic Worm S. Mansoniare Recognized Differently by the Innate Immune Receptor DC-SIGN

45. Targeting Galectins With Glycomimetics

46. Fluorinated carbohydrates as chemical probes formolecular recognition studies. Current statusand perspectives

47. The interaction of fluorinated glycomimetics with DC-SIGN: multiple binding modes disentangled by the combination of NMR methods and MD simulations

50. The Interaction of Fluorinated Glycomimetics with DC-SIGN: Multiple Binding Modes Disentangled by the Combination of NMR Methods and MD Simulations

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