Your search keyword '"Amato, Arianna"' showing total 2 results

1. Direct effect of infliximab on intestinal mucosa sustains mucosal healing: exploring new mechanisms of action.

Author

Petito, Valentina, Lopetuso, Loris Riccardo, Arena, Vincenzo, Stigliano, Egidio, Boninsegna, Alma, Bibbò, Stefano, Poscia, Andrea, Alfieri, Sergio, Rosa, Fausto, Amato, Arianna, Cammarota, Giovanni, Papa, Alfredo, Sgambato, Alessandro, Gasbarrini, Antonio, and Scaldaferri, Franco

Abstract

Background Infliximab is effective in inflammatory bowel disease through several mechanisms, possibly acting at the mucosal level. Aim To assess the role of infliximab on intestinal mucosa and whether it contributes to mucosal healing. Methods Human colonic mucosal biopsies were incubated with or without infliximab. Cultured biopsies were evaluated for histological staining, CD68, CD3, E-cadherin and phospho-extracellular signal-regulated kinases (ERK) expression, and apoptosis. A scratch assay and MTT assay were performed with Caco2 cells in the presence of infliximab and/or tumour necrosis factor (TNF)-α or treated with supernatants obtained from human peripheral blood mononuclear cells or human intestinal fibroblasts treated with TNF-α and infliximab alone or in association. Results Infliximab-treated biopsies displayed a better histological appearance, reduced inflammation with an increase of E-cadherin, phospho-ERK and apoptosis. Supernatants showed lower TNF-α, IL-17, IL-6 and IL-8 concentration, with an increase in fibroblast-growth-factor. Motility at scratch assay and proliferation at MTT assay of Caco2 cells displayed differential modulation by TNF-α and infliximab, directly or through supernatants of human intestinal fibroblasts and human peripheral blood mononuclear cells exposed to them. Conclusion Infliximab contributes to the mucosal healing process by acting directly at an intestinal mucosal level; infliximab indirectly affects epithelial cell migration and proliferation by acting on both fibroblasts and leukocytes. [ABSTRACT FROM AUTHOR]

Published

2016

2. Locally injected Infliximab ameliorates murine DSS colitis: Differences in serum and intestinal levels of drug between healthy and colitic mice.

Author

Lopetuso, Loris Riccardo, Petito, Valentina, Cufino, Valerio, Arena, Vincenzo, Stigliano, Egidio, Gerardi, Viviana, Gaetani, Eleonora, Poscia, Andrea, Amato, Arianna, Cammarota, Giovanni, Papa, Alfredo, Sgambato, Alessandro, Gasbarrini, Antonio, and Scaldaferri, Franco

Abstract

Abstract: Background: Infliximab is effective in human and murine IBD, but its pharmacodynamic is still poorly known. The aim of this study was to assess the affinity of infliximab to murine TNF-α, its role in murine colitis when administered intra-rectally and its levels in the blood, gut mucosa and stool of healthy and sick mice. Methods: An ELISA kit was built in order to assess the affinity of infliximab to human or murine-TNF-α. Human IgG were used as controls. DSS model of colitis on C57BL/6 mice was used to assess clinical efficacy of infliximab administered intravenously or by enema. Stool, serum and colon samples were collected to assess infliximab levels and histology for Rachmilewitz score. Results: Infliximab showed a good affinity both for human-TNF-α and murine-TNF-α. In DSS colitic mice infliximab ameliorated the severity of colitis, regardless of the administration route. In comparison with colitic mice, healthy mice displayed higher serum and mucosal infliximab levels, while detectable levels of infliximab were found in faeces, particularly in colitic mice. Conclusion: Our data support murine models to study infliximab pharmacokinetics and dynamics. Measurable levels of infliximab can be found at different concentrations in blood, intestinal mucosa and stool from healthy and sick mice, thus infliximab pharmacokinetics could have a major impact in human IBD. [Copyright &y& Elsevier]

Published

2013