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1. Human primary endothelial label-free biochip assay reveals unpredicted functions of plasma serine proteases

2. Neuronal Nitric Oxide Mediates the Anti-inflammatory Effects of Intestinal Ischemic Preconditioning

3. MASP-1 of the complement system alters fibrinolytic behaviour of blood clots

4. Novel MASP-2 inhibitors developed via directed evolution of human TFPI1 are potent lectin pathway inhibitors

5. Altered glycosylation of IgG4 promotes lectin complement pathway activation in anti-PLA2R1–associated membranous nephropathy

6. ITIH4 acts as a protease inhibitor by a novel inhibitory mechanism

7. Proprotein Convertase Is the Highest-Level Activator of the Alternative Complement Pathway in the Blood

8. Cutting Edge: A New Player in the Alternative Complement Pathway, MASP-1 Is Essential for LPS-Induced, but Not for Zymosan-Induced, Alternative Pathway Activation

9. Transcriptome analysis of inflammation-related gene expression in endothelial cells activated by complement MASP-1

10. Ligand-induced conformational rearrangements regulate the switch between membrane-proximal and distal functions of Rho kinase 2

11. Patterns of C1-Inhibitor/Plasma Serine Protease Complexes in Healthy Humans and in Hereditary Angioedema Patients

12. Key Components of the Complement Lectin Pathway Are Not Only Required for the Development of Inflammatory Arthritis but Also Regulate the Transcription of Factor D

13. Design and Selection of Novel C1s Inhibitors by In Silico and In Vitro Approaches

14. Contribution to the origin of Mn-U-Be-HREE-enrichment in phosphorite, near Bükkszentkereszt, NE Hungary

15. MASP-1 Increases Endothelial Permeability

16. MASP-1 and MASP-2 Do Not Activate Pro–Factor D in Resting Human Blood, whereas MASP-3 Is a Potential Activator: Kinetic Analysis Involving Specific MASP-1 and MASP-2 Inhibitors

17. MASP-1 of the complement system promotes clotting via prothrombin activation

18. Dissociation and re-association studies on the interaction domains of mannan-binding lectin (MBL)-associated serine proteases, MASP-1 and MASP-2, provide evidence for heterodimer formation

26. Intermodule cooperativity in the structure and dynamics of consecutive complement control modules in human C1r

27. Revisiting the mechanism of the autoactivation of the complement protease C1r in the C1 complex: Structure of the active catalytic region of C1r

28. MASP-1 Induced Clotting--The First Model of Prothrombin Activation by MASP-1

29. A True Autoactivating Enzyme

32. Assembly and Enzymatic Properties of the Catalytic Domain of Human Complement Protease C1r

33. Mirror image mutations reveal the significance of an intersubunit ion cluster in the stability of 3-isopropylmalate dehydrogenase

34. Functional effects of domain deletions in a multidomain serine protease, Clr

36. Cholesterol crystals activate the lectin complement pathway via ficolin-2 and MBL – Implications for the progression of atherosclerosis

38. Serpins and the Complement System

39. Biological variations of MASP-3 and MAp44, two splice products of the MASP1 gene involved in regulation of the complement system

40. Calcium-dependent conformational flexibility of a CUB domain controls activation of the complement serine protease C1r

41. Complement protease MASP-1 activates human endothelial cells: PAR4 activation is a link between complement and endothelial function

42. MASP-3 (MBL-associated serine protease 3)

43. Purification, crystallization and preliminary X-ray analysis of human mannose-binding lectin-associated serine protease-1 (MASP-1) catalytic region

44. MASP-1 (MBL-associated serine protease 1)

45. MASP-2 (MBL-associated serine protease 2)

46. Ecdysteroids increase the yield of recombinant protein produced in baculovirus insect cell expression system

47. Export signals

48. Serine proteases of the classical and lectin pathways: similarities and differences

49. The Initiation Complexes of the Classical and Lectin Pathways

50. Natural substrates and inhibitors of mannan-binding lectin-associated serine protease-1 and -2: a study on recombinant catalytic fragments

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