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31. The IbeA protein from adherent invasive Escherichia coli is a flavoprotein sharing structural homology with FAD-dependent oxidoreductases.

32. Molecular Actors of Inflammation and Their Signaling Pathways: Mechanistic Insights from Zebrafish.

34. Characterization of a member of the CEACAM protein family as a novel marker of proton pump-rich ionocytes on the zebrafish epidermis.

35. The receptor for advanced glycation end products is a sensor for cell-free heme.

36. Divalent cations influence the dimerization mode of murine S100A9 protein by modulating its disulfide bond pattern.

37. Structural Analysis of S100A8 Complex with Zinc and Calcium: A General Protocol for the Study of S100 Proteins in the Presence of Divalent Cations by X-Ray Crystallography.

38. A Single-Domain Antibody Targeting Complement Component C5 Acts as a Selective Inhibitor of the Terminal Pathway of the Complement System and Thus Functionally Mimicks the C-Terminal Domain of the Staphylococcus aureus SSL7 Protein.

39. [A cystein-dependent activation mechanism for the pro-inflammatory ligands of RAGE?]

40. The Structure of the RAGE:S100A6 Complex Reveals a Unique Mode of Homodimerization for S100 Proteins.

41. Crystal structure of human S100A8 in complex with zinc and calcium.

42. Structural basis for the targeting of complement anaphylatoxin C5a using a mixed L-RNA/L-DNA aptamer.

43. Structures and characterization of digoxin- and bufalin-bound Na+,K+-ATPase compared with the ouabain-bound complex.

44. Structural and functional characterization of human and murine C5a anaphylatoxins.

45. The specificity of DNA recognition by the RAGE receptor.

46. Structural insights into the oligomerization mode of the human receptor for advanced glycation end-products.

47. Structural insight on the recognition of surface-bound opsonins by the integrin I domain of complement receptor 3.

48. Crystal structure of the high-affinity Na+K+-ATPase-ouabain complex with Mg2+ bound in the cation binding site.

49. Human C3a and C3a desArg anaphylatoxins have conserved structures, in contrast to C5a and C5a desArg.

50. Structural basis for activation of the complement system by component C4 cleavage.

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