Your search keyword '"Stefani, Annalisa"' showing total 3 results

1. Neuropeptide neurotensin stimulates intestinal wound healing following chronic intestinal inflammation

Author

Brun, Paola, Mastrotto, Cristina, Beggiao, Elisa, Stefani, Annalisa, Barzon, Luisa, Sturniolo, Giacomo C., Palu, Giorgio, and Castagliuolo, Ignazio

Subjects

Neuropeptides -- Research, Neuropeptides -- Physiological aspects, Neurotensin -- Research, Neurotensin -- Physiological aspects, Colorectal diseases -- Research, Colorectal diseases -- Care and treatment, Gastrointestinal diseases -- Research, Gastrointestinal diseases -- Care and treatment, Biological sciences

Abstract

Because neurotensin (NT) and its high-affinity receptor (NTR1) modulate immune responses, chloride secretion, and epithelial cell proliferation, we sought to investigate their role in the repair process that follows the development of mucosal injuries during a persistent inflammation. Colonic NT and NTR1, mRNA, and protein significantly increased only after dextran sodium sulfate (DSS)-induced inflammatory damage developed. Colitis-induced body weight loss, colonic myeloperoxidase activity, and histological damage were significantly enhanced by SR-48642 administration, a nonpeptide NTR1 antagonist, whereas continuous NT infusion ameliorated colitis outcome. To evaluate the NT and NTR1 role in tissue healing, mucosal inflammatory injury was established administering 3% DSS for 5 days. After DSS discontinuation, mice rapidly gained weight, ulcers were healed, and colonic NT, NTR1, and cyclooxygenase (COX)-2 mRNA levels were upregulated, whereas SR-48642 treatment caused a further body weight loss, ulcer enlargement, and a blunted colonic COX-2 mRNA upregulation. In a wound-healing model in vitro, NT-induced cell migration in the denuded area was inhibited by indomethacin but not by an antitransforming growth factor-J3 neutralizing antibody. Furthermore, NT significantly increased COX-2 mRNA levels by 2.4-fold and stimulated PG[E.sub.2] release in HT-29 cells. These findings suggest that NT and NTR1 are part of the network activated after mucosal injuries and that NT stimulates epithelial restitution at least, in part, through a COX-2 dependent pathway. neurotensin receptor type 1; healing; colitis; cyclooxygenase-2; inflammatory bowel disease

Published

2005

2. Snail1 transcription factor is a critical mediator of hepatic stellate cell activation following hepatic injury

Author

Scarpa, Melania, primary, Grillo, Alessia R., additional, Brun, Paola, additional, Macchi, Veronica, additional, Stefani, Annalisa, additional, Signori, Sara, additional, Buda, Andrea, additional, Fabris, Paolo, additional, Giordani, Maria Teresa, additional, De Caro, Raffaele, additional, Palù, Giorgio, additional, Castagliuolo, Ignazio, additional, and Martines, Diego, additional

Published

2011

3. Snail1 transcription factor is a critical mediator of hepatic stellate cell activation following hepatic injury.

Author

Scarpa M, Grillo AR, Brun P, Macchi V, Stefani A, Signori S, Buda A, Fabris P, Giordani MT, De Caro R, Palù G, Castagliuolo I, and Martines D

Subjects

Acute Disease, Adult, Aged, Animals, Blotting, Western, Carbon Tetrachloride, Cell Transdifferentiation, Cells, Cultured, Chronic Disease, Gene Silencing, Hepatic Stellate Cells pathology, Humans, Immunologic Techniques, Liver pathology, Liver physiopathology, Liver Cirrhosis chemically induced, Mice, Middle Aged, Reverse Transcriptase Polymerase Chain Reaction methods, Snail Family Transcription Factors, Thioacetamide, Up-Regulation, Wound Healing, Hepatic Stellate Cells metabolism, Liver Cirrhosis pathology, Liver Cirrhosis physiopathology, Transcription Factors metabolism

Abstract

Following liver injury, the wound-healing process is characterized by hepatic stellate cell (HSC) activation from the quiescent fat-storing phenotype to a highly proliferative myofibroblast-like phenotype. Snail1 is a transcription factor best known for its ability to trigger epithelial-mesenchymal transition, to influence mesoderm formation during embryonic development, and to favor cell survival. In this study, we evaluated the expression of Snail1 in experimental and human liver fibrosis and analyzed its role in the HSC transdifferentiation process. Liver samples from patients with liver fibrosis and from mice treated by either carbon tetrachloride (CCl(4)) or thioacetamide (TAA) were evaluated for mRNA expression of Snail1. The transcription factor expression was investigated by immunostaining and real-time quantitative RT-PCR (qRT-PCR) on in vitro and in vivo activated murine HSC. Snail1 knockdown studies on cultured HSC and on CCl(4)-treated mice were performed by adenoviral delivery of short-hairpin RNA; activation-related genes were quantitated by real-time qRT-PCR and Western blotting. Snail1 mRNA expression resulted upregulated in murine experimental models of liver injury and in human hepatic fibrosis. In vitro studies showed that Snail1 is expressed by HSC and that its transcription is augmented in in vitro and in vivo activated HSC compared with quiescent HSC. At the protein level, we could observe the nuclear translocation of Snail1 in activated HSC. Snail1 knockdown resulted in the downregulation of activation-related genes both in vitro and in vivo. Our data support a role for Snail1 transcription factor in the hepatic wound-healing response and its involvement in the HSC transdifferentiation process.

Published

2011