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1. Inhibitor of NF-kappa B kinases alpha and beta are both essential for high mobility group box 1-mediated chemotaxis

3. Group IIA secreted phospholipase A2 is associated with the pathobiology leading to COVID-19 mortality.

4. Group IIA Secreted Phospholipase A 2 Plays a Central Role in the Pathobiology of COVID-19.

5. The Vitamin D Binding Protein and Inflammatory Injury: A Mediator or Sentinel of Tissue Damage?

6. Vitamin D-binding protein deficiency in mice decreases systemic and select tissue levels of inflammatory cytokines in a murine model of acute muscle injury.

7. Loss of acid ceramidase in myeloid cells suppresses intestinal neutrophil recruitment.

9. Sphingolipids in neutrophil function and inflammatory responses: Mechanisms and implications for intestinal immunity and inflammation in ulcerative colitis.

10. Identification of the gC1qR sites for the HIV-1 viral envelope protein gp41 and the HCV core protein: Implications in viral-specific pathogenesis and therapy.

11. Enhanced recognition of plasma proteins in a non-native state by complement C3b. A possible clearance mechanism for damaged proteins in blood.

12. Cell migration to CXCL12 requires simultaneous IKKα and IKKβ-dependent NF-κB signaling.

13. Circulating complexes of the vitamin D binding protein with G-actin induce lung inflammation by targeting endothelial cells.

14. Generation of multiple fluid-phase C3b:plasma protein complexes during complement activation: possible implications in C3 glomerulopathies.

15. Soluble gC1qR is an autocrine signal that induces B1R expression on endothelial cells.

16. Neutrophil recruitment to the lung in both C5a- and CXCL1-induced alveolitis is impaired in vitamin D-binding protein-deficient mice.

17. The IKKα-dependent NF-κB p52/RelB noncanonical pathway is essential to sustain a CXCL12 autocrine loop in cells migrating in response to HMGB1.

18. Cofactor regulation of C5a chemotactic activity in physiological fluids. Requirement for the vitamin D binding protein, thrombospondin-1 and its receptors.

19. DNA alkylating therapy induces tumor regression through an HMGB1-mediated activation of innate immunity.

20. Identification of two distinct cell binding sequences in the vitamin D binding protein.

21. Inhibitor of NF-kappa B kinases alpha and beta are both essential for high mobility group box 1-mediated chemotaxis [corrected].

22. Upregulation of vitamin D binding protein (Gc-globulin) binding sites during neutrophil activation from a latent reservoir in azurophil granules.

23. Selective inhibition of the C5a chemotactic cofactor function of the vitamin D binding protein by 1,25(OH)2 vitamin D3.

24. Chemotaxis of human monocyte-derived dendritic cells to complement component C1q is mediated by the receptors gC1qR and cC1qR.

25. CD44 and annexin A2 mediate the C5a chemotactic cofactor function of the vitamin D binding protein.

26. Identification of a region in the vitamin D-binding protein that mediates its C5a chemotactic cofactor function.

27. Protease-activated receptor-2 (PAR-2) expression in human fibroblasts is regulated by growth factors and extracellular matrix.

28. Platelet-derived thrombospondin-1 is necessary for the vitamin D-binding protein (Gc-globulin) to function as a chemotactic cofactor for C5a.

29. The differentiation and function of myofibroblasts is regulated by mast cell mediators.

30. Elastase controls the binding of the vitamin D-binding protein (Gc-globulin) to neutrophils: a potential role in the regulation of C5a co-chemotactic activity.

31. Mast cell tryptase does not alter matrix metalloproteinase expression in human dermal fibroblasts: further evidence that proteolytically-active tryptase is a potent fibrogenic factor.

32. Initial characterization of the complement activating compounds in extracts of smokeless tobacco.

33. Initial characterization of the vitamin D binding protein (Gc-globulin) binding site on the neutrophil plasma membrane: evidence for a chondroitin sulfate proteoglycan.

34. Smokeless tobacco extracts activate complement in vitro: a potential pathogenic mechanism for initiating inflammation of the oral mucosa.

35. Human mast cells activate fibroblasts: tryptase is a fibrogenic factor stimulating collagen messenger ribonucleic acid synthesis and fibroblast chemotaxis.

36. Undifferentiated U937 cells transfected with chemoattractant receptors: a model system to investigate chemotactic mechanisms and receptor structure/function relationships.

37. Elevated levels of 92-kd type IV collagenase (matrix metalloproteinase 9) in giant cell arteritis.

38. Markedly elevated serum MMP-9 (gelatinase B) levels in rheumatoid arthritis: a potentially useful laboratory marker.

39. Co-chemotactic effect of Gc-globulin (vitamin D binding protein) for C5a. Transient conversion into an active co-chemotaxin by neutrophils.

40. Inhibition of neutrophil chemotaxis by protease inhibitors. Differential effect of inhibitors of serine and thiol proteases.

41. Murine mast cells express two types of C1q receptors that are involved in the induction of chemotaxis and chemokinesis.

42. Borrelia burgdorferi binds plasminogen, resulting in enhanced penetration of endothelial monolayers.

43. Binding of Gc globulin (vitamin D binding protein) to C5a or C5a des Arg is not necessary for co-chemotactic activity.

44. Transforming growth factor-beta 1 mediates mast cell chemotaxis.

45. Human neutrophil Fc gamma RIIIB and formyl peptide receptors are functionally linked during formyl-methionyl-leucyl-phenylalanine-induced chemotaxis.

46. Priming of human neutrophil functions by tumor necrosis factor: enhancement of superoxide anion generation, degranulation, and chemotaxis to chemoattractants C5a and F-Met-Leu-Phe.

47. Ceruloplasmin and transferrin levels are altered in serum and bronchoalveolar lavage fluid of patients with the adult respiratory distress syndrome.

48. Concentration-dependent regulatory effects of prostaglandin E1 on human neutrophil function in vitro.

49. Regulation of neutrophil function by acute phase reactants. Implications for resolution of the adult respiratory distress syndrome.

50. Human C-reactive protein inhibits neutrophil chemotaxis in vitro: possible implications for the adult respiratory distress syndrome.

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