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7 results on '"Durigutto P"'

1. 'Fluvastatin treatment inhibits leucocyte adhesion and extravasation in models of complement-mediated acute inflamation'F.Fischetti, R. Carretta, G. Borotto, P. Durigutto, R. Bulla, P.L. Meroni, F. Tedesco

Author

FISCHETTI, Fabio, CARRETTA, RENZO, Borotto G., Durigutto P., BULLA, ROBERTA, Meroni P.L., Tedesco F., Fischetti, Fabio, Carretta, Renzo, Borotto, G., Durigutto, P., Bulla, Roberta, Meroni, P. L., and Tedesco, F.

Subjects
Fluvastatin, leucocyte adhesion, complement
Abstract

Complement activation plays a relevant role in the development of tissue damage under inflammatory conditions, and clinical and experimental observations emphasize its contribution to inflammatory vasculitides. Statins have recently been shown to reduce cardiovascular morbidity independently of plasma cholesterol lowering and in vitro studies support a direct anti-inflammatory action of these drugs. The aim of this study was to verify the in vivo effect of fluvastatin on complement-mediated acute peritoneal inflammation. The effect of oral treatment with fluvastatin was investigated in normo-cholesterolaemic rats that received intraperitoneal injection of either yeast-activated rat serum (Y-act RS) or lipopolysaccharide to induce peritoneal inflammation monitored by the number of PMN recruited in peritoneal fluid washes. In addition, vascular adherence and extravasation of leucocytes were evaluated by direct videomicroscopy examination on mesentery postcapillary venules topically exposed to Y-act RS. The number of PMN in the peritoneal washes of rats treated with fluvastatin was 38% lower than that of untreated animals (P < 0.05) 12 h after LPS injection, and was even lower (56%) in rats treated with Y-act RS already 8 h after injection (P < 0.02). Firm adhesion to endothelium and extravasation of leucocytes evaluated under direct videomicroscopy observation were significantly inhibited in fluvastatin treated rats (77% and 72%, respectively; P < 0.01), 120 min after treatment with Y-act RS. Our results demonstrate that fluvastatin inhibits in vivo complement-dependent acute peritoneal inflammation and suggest a role for statins in preventing the inflammatory flares usually associated with complement activation in chronic diseases, such as SLE or rheumatoid arthritis.

Published
2004

3. Fluvastatin treatment inhibits leucocyte adhesion and extravasation in models of complement-mediated acute inflammation.

Author

Fischetti, F., Carretta, R., Borotto, G., Durigutto, P., Bulla, R., Meroni, P. L., and Tedesco, F.

Subjects
VASCULITIS, KILLER cells, ENZYME activation, STATINS (Cardiovascular agents), INTRAPERITONEAL injections, ISOPENTENOIDS, CHRONIC diseases, ENDOTHELIUM, MESENTERY, RHEUMATOID arthritis, LEUCOCYTES, SYSTEMIC lupus erythematosus
Abstract

Complement activation plays a relevant role in the development of tissue damage under inflammatory conditions, and clinical and experimental observations emphasize its contribution to inflammatory vasculitides. Statins have recently been shown to reduce cardiovascular morbidity independently of plasma cholesterol lowering and in vitro studies support a direct anti-inflammatory action of these drugs. The aim of this study was to verify the in vivo effect of fluvastatin on complement-mediated acute peritoneal inflammation. The effect of oral treatment with fluvastatin was investigated in normo-cholesterolaemic rats that received intraperitoneal injection of either yeast-activated rat serum (Y-act RS) or lipopolysaccharide to induce peritoneal inflammation monitored by the number of PMN recruited in peritoneal fluid washes. In addition, vascular adherence and extravasation of leucocytes were evaluated by direct videomicroscopy examination on mesentery postcapillary venules topically exposed to Y-act RS. The number of PMN in the peritoneal washes of rats treated with fluvastatin was 38% lower than that of untreated animals ( P < 0·05) 12 h after LPS injection, and was even lower (56%) in rats treated with Y-act RS already 8 h after injection ( P < 0·02). Firm adhesion to endothelium and extravasation of leucocytes evaluated under direct videomicroscopy observation were significantly inhibited in fluvastatin treated rats (77% and 72%, respectively; P < 0·01), 120 min after treatment with Y-act RS. Our results demonstrate that fluvastatin inhibits in vivo complement-dependent acute peritoneal inflammation and suggest a role for statins in preventing the inflammatory flares usually associated with complement activation in chronic diseases, such as SLE or rheumatoid arthritis. [ABSTRACT FROM AUTHOR]

Published
2004
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4. Mannose-binding lectin is produced by vaginal epithelial cells and its level in the vaginal fluid is influenced by progesterone

Author

Bulla, R., De Seta, F., Radillo, O., Agostinis, C., Durigutto, P., Pellis, V., De Santo, D., Crovella, S., and Tedesco, F.

Subjects
*MANNOSE, *LECTINS, *EPITHELIAL cells, *BODY fluids, *PROGESTERONE, *PATHOGENIC bacteria, *VAGINA, *FEMALE reproductive organs
Abstract

Abstract: Mannose-binding lectin (MBL) is a recognition molecule of the complement (C) system and binds to carbohydrate ligands present on a wide range of pathogenic bacteria, viruses, fungi, and parasites. MBL has been detected in the cervico-vaginal cavity where it can provide a first-line defence against infectious agents colonizing the lower tract of the reproductive system. Analysis of the cervico-vaginal lavage (CVL) obtained from 11 normal cycling women at different phases of the menstrual cycle revealed increased levels of MBL in the secretive phase. Part of this MBL derives from the circulation as indicated by the presence of transferrin in CVL tested as a marker of vascular and tissue permeability. The local synthesis of MBL is suggested by the finding that its level is substantially higher than that of transferrin in the secretive phase. The contribution of endometrium is negligible since the MBL level did not change before and after hysterectomy. RT-PCR and in situ RT-PCR analysis showed that the vaginal tissue, and in particular the basal layer of the epithelium, is a source of MBL which binds to the basal membrane and to cells of the outer layers of the epithelium. In conclusion, we have shown that MBL detected in CVL derives both from plasma as result of transudation and from local synthesis and its level is progesterone dependent increasing in the secretive phase of the menstrual cycle. [ABSTRACT FROM AUTHOR]

Published
2010
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5. Treatment of experimental arthritis by targeting synovial endothelium with a neutralizing recombinant antibody to C5

Author

Costantino Pitzalis, Chiara Garrovo, Paolo Durigutto, Luca De Maso, Andrea Cortini, Paolo Macor, Daniele Sblattero, Stefania Biffi, Roberto Marzari, Francesco Tedesco, Fabio Fischetti, Macor, Paolo, Durigutto, P, De Maso, L, Garrovo, C, Biffi, S, Cortini, A, Fischetti, Fabio, Sblattero, Daniele, Pitzalis, C, Marzari, Roberto, and Tedesco, Francesco

Subjects
Male, Freund's Adjuvant, Arthritis, Mice, Immunology and Allergy, complement, Pharmacology (medical), Neutralizing antibody, Complement component 5, Mice, Inbred BALB C, biology, Synovial Membrane, Complement C5, imaging, Serum Albumin, Bovine, Recombinant Proteins, animal models, arthriti, medicine.anatomical_structure, arthritis, Rheumatoid arthritis, Tumor necrosis factor alpha, Collagen, medicine.symptom, musculoskeletal diseases, Immunology, Inflammation, Rheumatology, In vivo, medicine, Animals, Humans, Endothelium, biologic therapy, Rats, Wistar, Interleukin-6, Tumor Necrosis Factor-alpha, business.industry, animal model, medicine.disease, Antibodies, Neutralizing, Arthritis, Experimental, Rats, Disease Models, Animal, biology.protein, Synovial membrane, business
Abstract

Objective To show that a new recombinant protein (MT07) obtained by fusing a synovial-homing peptide to a neutralizing antibody to C5 can be selectively delivered to inflamed synovium and can effectively control joint inflammation in experimental models of arthritis. Methods Binding of MT07 to human, rat, and mouse synovial tissue was evaluated in vitro by immunofluorescence, and selective localization in the inflamed joints of rats was documented in vivo using time-domain optical imaging. The antiinflammatory effect of MT07 was tested in a rat model of antigen-induced arthritis (AIA) and in a mouse model of collagen antibody–induced arthritis (CAIA). Results MT07 was able to bind to samples of inflamed synovium from humans, mice, and rats while failing to recognize uninflamed synovium as well as inflamed mouse lung or rat kidney. In vivo analysis of the biodistribution of MT07 confirmed its preferential homing to inflamed joints, with negligible inhibition of circulating C5 levels. MT07 prevented and resolved established inflammation in a rat model of AIA, as demonstrated by changes in joint swelling, polymorphonuclear cell counts in synovial washes, release of interleukin-6 and tumor necrosis factor α, and tissue damage. A similar therapeutic effect was obtained testing MT07 in a CAIA model. Conclusion Our findings show that the novel recombinant molecule MT07 has the unique ability to selectively target inflamed joints and to exert local control of the inflammatory process by neutralizing the complement system without interfering with circulating C5 levels. We believe that this approach can be extended to other antiinflammatory drugs currently used to treat patients with rheumatoid arthritis.

Published
2012
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6. Innate immunity, through late complement components activation, contributes to the development of early vascular inflammation and morphologic alterations in experimental diabetes

Author

Riccardo Candido, Barbara Toffoli, Stella Bernardi, Francesco Tedesco, Paolo Durigutto, Renzo Carretta, Fabio Fischetti, Bruno Fabris, Fischetti, Fabio, Candido, Riccardo, Toffoli, Barbara, Durigutto, P., Bernardi, Stella, Carretta, Renzo, Tedesco, Francesco, and Fabris, Bruno

Subjects
Male, Time Factors, medicine.medical_treatment, Blood Pressure, Complement Membrane Attack Complex, Extracellular matrix, vascular, Transforming Growth Factor beta, Innate, complement, Complement Activation, Platelet-Derived Growth Factor, Microscopy, Video, Cell adhesion molecule, Complement C3, Complement C9, Complement C6, Extracellular Matrix, Mesenteric Arteries, Vascular endothelial growth factor B, medicine.symptom, Inflammation Mediators, Rats, Transgenic, Cardiology and Cardiovascular Medicine, Platelet-derived growth factor receptor, medicine.medical_specialty, immunity, inflammation, Vascular Cell Adhesion Molecule-1, Inflammation, Biology, Diabetes Mellitus, Experimental, Internal medicine, Proliferating Cell Nuclear Antigen, medicine, Animals, Leukocyte Rolling, Rats, Wistar, Analysis of Variance, Growth factor, Connective Tissue Growth Factor, Hypertrophy, Atherosclerosis, Immunity, Innate, Rats, CTGF, Endocrinology, Gene Expression Regulation, biology.protein, Diabetic Angiopathies, Transforming growth factor
Abstract

Objective To verify if innate immunity, and namely the assembly of terminal complement complex (TCC) could be involved in the development of early diabetic vascular damage. Methods and results At first in 2 groups of diabetic or non-diabetic Wistar rats the occurrence of basal or stimulated stable adherence to the endothelial layer and extravasation of circulating fluorescently-labelled leukocytes was assessed by using an in vivo videomicroscopy technique. In a second part of the study, the development of vascular damage in short term diabetes was studied in the genetically C6 deficient rats of the PVG strain, and compared with those observed in the wild-type C6 sufficient animals. Here, the analysis of mesentery vascular expression of mRNA for vascular cell adhesion molecule (VCAM)-1, transforming growth factor-β (TGF-β), connective tissue growth factor (CTGF), and platelet-derived growth factor (PDGF), the evaluation of intravascular protein levels of VCAM-1, TGF-β, CTGF, proliferative cell nuclear antigen (PCNA), as well as the assessment of structural changes and Complement components deposition at the mesentery arterial vascular wall were also performed. Conclusions Leukocyte trafficking, mesentery arteries hypertrophy, extracellular matrix deposition, local vascular gene and protein expression of VCAM-1, TGF-β, CTGF and PCNA, as well as PGDF gene expression were all increased by short term diabetes, but all significantly reduced in the C6 deficient diabetic animals, thus suggesting an active role for TCC in the development of vascular inflammation in the early phases of experimental diabetes.

Published
2010

7. Novel pathogenic mechanism and therapeutic approaches to angioedema associated with C1 inhibitor deficiency

Author

Marco Cicardi, Barbara Frossi, Paolo Durigutto, Ellinor I.B. Peerschke, Domenico Regoli, Fabio Fischetti, Fleur Bossi, Fernand Gobeil, Berhane Ghebrehiwet, Francesco Tedesco, Bossi, Fleur, Fischetti, Fabio, Regoli, D., Durigutto, P., Frossi, B., Gobeil, F. J. r., Ghebrehiwet, B., Peerschke, E. I., Cicardi, M., and Tedesco, Francesco

Subjects
Male, medicine.medical_specialty, Immunology, Adrenergic beta-Antagonists, Interleukin-1beta, Bradykinin, angioedema, complement, therapy, Vascular permeability, Receptor, Bradykinin B1, Rats, Inbred WKY, Article, C1-inhibitor, Capillary Permeability, chemistry.chemical_compound, Icatibant, Internal medicine, Cell Line, Tumor, medicine, Immunology and Allergy, Animals, Humans, Immunologic Factors, Receptor, Protein Synthesis Inhibitors, Kininogen, Brefeldin A, Membrane Glycoproteins, Angioedema, biology, Hereditary Angioedema Types I and II, Antibodies, Monoclonal, medicine.disease, Rats, Receptors, Complement, Bradykinin B1 Receptor Antagonists, Endocrinology, chemistry, Hereditary angioedema, biology.protein, Blood Vessels, medicine.symptom, Complement C1 Inhibitor Protein
Abstract

Background Activation of bradykinin-mediated B2 receptor has been shown to play an important role in the onset of angioedema associated with C1 inhibitor deficiency. This finding has led to the development of novel therapeutic drugs such as the B2 receptor antagonist icatibant. However, it is unclear whether other receptors expressed on endothelial cells contribute to the release of kinins and vascular leakage in these patients. The recognition of their role may have obvious therapeutic implications. Objective Our aim was to investigate the involvement of B1 and gC1q receptors in in vitro and in vivo models of vascular leakage induced by plasma samples obtained from patients with C1 inhibitor deficiency. Methods The vascular leakage was evaluated in vitro on endothelial cells by a transwell model system and in vivo on rat mesentery microvessels by intravital microscopy. Results We observed that the attack phase plasma from C1 inhibitor–deficient patients caused a delayed fluorescein-labeled albumin leakage as opposed to the rapid effect of bradykinin, whereas remission plasma elicited a modest effect compared with control plasma. The plasma permeabilizing effect was prevented by blocking the gC1q receptor–high-molecular-weight kininogen interaction, was partially inhibited by B2 receptor or B1 receptor antagonists, and was totally prevented by the mixture of the 2 antagonists. Involvement of B1 receptor was supported by the finding that albumin leakage caused by attack phase plasma was enhanced by IL-1β and was markedly reduced by brefeldin A. Conclusion Our data suggest that both B1 receptor and gC1q receptor are involved in the vascular leakage induced by hereditary and acquired angioedema plasma.

Published
2009

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