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1. (Re) Solving Repair After Myocardial Infarction

2. Melanocortin Peptide Therapy for the Treatment of Arthritic Pathologies

3. Ly6C high Monocytes Oscillate in the Heart During Homeostasis and After Myocardial Infarction—Brief Report

4. Macrophage-derived IL-10 mediates mucosal repair by epithelial WISP-1 signaling

5. The advantageous role of annexin A1 in cardiovascular disease

6. Annexin A1: shifting the balance towards resolution and repair

7. Pro-Angiogenic Macrophage Phenotype to Promote Myocardial Repair

8. Ly6C

9. Neutrophil-derived JAML inhibits repair of intestinal epithelial injury during acute inflammation

10. Redox signaling regulates commensal-mediated mucosal homeostasis and restitution and requires formyl peptide receptor 1

11. Annexin A2 Regulates β1 Integrin Internalization and Intestinal Epithelial Cell Migration

12. Annexin A1, formyl peptide receptor, and NOX1 orchestrate epithelial repair

13. Antiallergic Cromones Inhibit Neutrophil Recruitment Onto Vascular Endothelium via Annexin-A1 Mobilization

14. The melanocortin MC1 receptor agonist BMS-470539 inhibits leucocyte trafficking in the inflamed vasculature

15. Melanocortin Peptide Therapy for the Treatment of Arthritic Pathologies

16. Inflamed phenotype of the mesenteric microcirculation of melanocortin type 3 receptor‐null mice after ischemia‐reperfusion

17. The microenvironment of injured murine gut elicits a local pro-restitutive microbiota

18. Wound repair: role of immune–epithelial interactions

19. Cutting Edge: IL-36 Receptor Promotes Resolution of Intestinal Damage

20. The Microenvironment of Injured Mucosa Stimulates a Local Pro‐restitutive Microbiota

22. Annexin A1-containing extracellular vesicles and polymeric nanoparticles promote epithelial wound repair

23. [d-Trp8]-γ-Melanocyte-Stimulating Hormone Exhibits Anti-Inflammatory Efficacy in Mice Bearing a Nonfunctional MC1R (Recessive Yellow e/e Mouse)

24. Annexin 1 and Melanocortin Peptide Therapy for Protection Against Ischaemic-Reperfusion Damage in the Heart

25. Recruitment of classical monocytes can be inhibited by disturbing heteromers of neutrophil HNP1 and platelet CCL5

26. Annexin A1 Counteracts Chemokine-Induced Arterial Myeloid Cell Recruitment

29. Enteric commensal bacteria activate formyl peptide receptor 1 to regulate intestinal epithelial homeostasis and wound repair (488.7)

30. Evidence for a role of p130Cas in JAM‐A‐dependent signaling events (60.3)

31. Annexin A1 released from epithelial extracellular vesicles and synthetic nanoparticles promotes wound repair (488.5)

32. JAM-A associates with ZO-2, afadin, and PDZ-GEF1 to activate Rap2c and regulate epithelial barrier function

33. The N-BAR Domain Protein, Bin3, Regulates Rac1- and Cdc42-Dependent Processes in Myogenesis

36. JAM‐A –mediated regulation of epithelial barrier function is dependent on a complex with ZO‐2, Afadin and PDZ‐GEF1 that modulates Rap2c activity

37. Epithelial wound repair: insights into the multifaceted roles of Annexin A1

38. Distinct phospholipase C-β isozymes mediate lysophosphatidic acid receptor 1 effects on intestinal epithelial homeostasis and wound closure

39. O-012 The Intestinal Wound Regeneration Modulates Mucosal Microenvironment to Stimulate Expansion of a Local Pro-restitutive Microbiota

43. Melanocortin control of cell trafficking in vascular inflammation

44. Cell Adhesion Molecules

45. Inflammation-dependent alpha 5 beta 1 (very late antigen-5) expression on leukocytes reveals a functional role for this integrin in acute peritonitis

46. Melanocortin Control of Cell Trafficking in Vascular Inflammation

50. CAR-dependent intestinal epithelial wound repair is inhibited by JAML released from migrating neutrophils (P4047)

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