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Characterization of Early and Late Damage in a Mouse Model of Pelvic Radiation Disease

Pelvic radiation disease (PRD), a frequent side effect in patients with abdominal/pelvic cancers treated with radiotherapy, remains an unmet medical need. Currently available preclinical models have limited applications for the investigation of PRD pathogenesis and possible therapeutic strategies. I...

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Autores principales: Vitali, Roberta, Palone, Francesca, De Stefano, Ilaria, Fiorente, Chiara, Novelli, Flavia, Pasquali, Emanuela, Fratini, Emiliano, Tanori, Mirella, Leonardi, Simona, Tanno, Barbara, Colantoni, Eleonora, Soldi, Sara, Galletti, Serena, Grimaldi, Maria, Morganti, Alessio Giuseppe, Fuccio, Lorenzo, Pazzaglia, Simonetta, Pioli, Claudio, Mancuso, Mariateresa, Vesci, Loredana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10218716/
https://www.ncbi.nlm.nih.gov/pubmed/37240150
http://dx.doi.org/10.3390/ijms24108800
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author Vitali, Roberta
Palone, Francesca
De Stefano, Ilaria
Fiorente, Chiara
Novelli, Flavia
Pasquali, Emanuela
Fratini, Emiliano
Tanori, Mirella
Leonardi, Simona
Tanno, Barbara
Colantoni, Eleonora
Soldi, Sara
Galletti, Serena
Grimaldi, Maria
Morganti, Alessio Giuseppe
Fuccio, Lorenzo
Pazzaglia, Simonetta
Pioli, Claudio
Mancuso, Mariateresa
Vesci, Loredana
author_facet Vitali, Roberta
Palone, Francesca
De Stefano, Ilaria
Fiorente, Chiara
Novelli, Flavia
Pasquali, Emanuela
Fratini, Emiliano
Tanori, Mirella
Leonardi, Simona
Tanno, Barbara
Colantoni, Eleonora
Soldi, Sara
Galletti, Serena
Grimaldi, Maria
Morganti, Alessio Giuseppe
Fuccio, Lorenzo
Pazzaglia, Simonetta
Pioli, Claudio
Mancuso, Mariateresa
Vesci, Loredana
author_sort Vitali, Roberta
collection PubMed
description Pelvic radiation disease (PRD), a frequent side effect in patients with abdominal/pelvic cancers treated with radiotherapy, remains an unmet medical need. Currently available preclinical models have limited applications for the investigation of PRD pathogenesis and possible therapeutic strategies. In order to select the most effective irradiation protocol for PRD induction in mice, we evaluated the efficacy of three different locally and fractionated X-ray exposures. Using the selected protocol (10 Gy/day × 4 days), we assessed PRD through tissue (number and length of colon crypts) and molecular (expression of genes involved in oxidative stress, cell damage, inflammation, and stem cell markers) analyses at short (3 h or 3 days after X-ray) and long (38 days after X-rays) post-irradiation times. The results show that a primary damage response in term of apoptosis, inflammation, and surrogate markers of oxidative stress was found, thus determining a consequent impairment of cell crypts differentiation and proliferation as well as a local inflammation and a bacterial translocation to mesenteric lymph nodes after several weeks post-irradiation. Changes were also found in microbiota composition, particularly in the relative abundance of dominant phyla, related families, and in alpha diversity indices, as an indication of dysbiotic conditions induced by irradiation. Fecal markers of intestinal inflammation, measured during the experimental timeline, identified lactoferrin, along with elastase, as useful non-invasive tools to monitor disease progression. Thus, our preclinical model may be useful to develop new therapeutic strategies for PRD treatment.
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spelling pubmed-102187162023-05-27 Characterization of Early and Late Damage in a Mouse Model of Pelvic Radiation Disease Vitali, Roberta Palone, Francesca De Stefano, Ilaria Fiorente, Chiara Novelli, Flavia Pasquali, Emanuela Fratini, Emiliano Tanori, Mirella Leonardi, Simona Tanno, Barbara Colantoni, Eleonora Soldi, Sara Galletti, Serena Grimaldi, Maria Morganti, Alessio Giuseppe Fuccio, Lorenzo Pazzaglia, Simonetta Pioli, Claudio Mancuso, Mariateresa Vesci, Loredana Int J Mol Sci Article Pelvic radiation disease (PRD), a frequent side effect in patients with abdominal/pelvic cancers treated with radiotherapy, remains an unmet medical need. Currently available preclinical models have limited applications for the investigation of PRD pathogenesis and possible therapeutic strategies. In order to select the most effective irradiation protocol for PRD induction in mice, we evaluated the efficacy of three different locally and fractionated X-ray exposures. Using the selected protocol (10 Gy/day × 4 days), we assessed PRD through tissue (number and length of colon crypts) and molecular (expression of genes involved in oxidative stress, cell damage, inflammation, and stem cell markers) analyses at short (3 h or 3 days after X-ray) and long (38 days after X-rays) post-irradiation times. The results show that a primary damage response in term of apoptosis, inflammation, and surrogate markers of oxidative stress was found, thus determining a consequent impairment of cell crypts differentiation and proliferation as well as a local inflammation and a bacterial translocation to mesenteric lymph nodes after several weeks post-irradiation. Changes were also found in microbiota composition, particularly in the relative abundance of dominant phyla, related families, and in alpha diversity indices, as an indication of dysbiotic conditions induced by irradiation. Fecal markers of intestinal inflammation, measured during the experimental timeline, identified lactoferrin, along with elastase, as useful non-invasive tools to monitor disease progression. Thus, our preclinical model may be useful to develop new therapeutic strategies for PRD treatment. MDPI 2023-05-15 /pmc/articles/PMC10218716/ /pubmed/37240150 http://dx.doi.org/10.3390/ijms24108800 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Vitali, Roberta
Palone, Francesca
De Stefano, Ilaria
Fiorente, Chiara
Novelli, Flavia
Pasquali, Emanuela
Fratini, Emiliano
Tanori, Mirella
Leonardi, Simona
Tanno, Barbara
Colantoni, Eleonora
Soldi, Sara
Galletti, Serena
Grimaldi, Maria
Morganti, Alessio Giuseppe
Fuccio, Lorenzo
Pazzaglia, Simonetta
Pioli, Claudio
Mancuso, Mariateresa
Vesci, Loredana
Characterization of Early and Late Damage in a Mouse Model of Pelvic Radiation Disease
title Characterization of Early and Late Damage in a Mouse Model of Pelvic Radiation Disease
title_full Characterization of Early and Late Damage in a Mouse Model of Pelvic Radiation Disease
title_fullStr Characterization of Early and Late Damage in a Mouse Model of Pelvic Radiation Disease
title_full_unstemmed Characterization of Early and Late Damage in a Mouse Model of Pelvic Radiation Disease
title_short Characterization of Early and Late Damage in a Mouse Model of Pelvic Radiation Disease
title_sort characterization of early and late damage in a mouse model of pelvic radiation disease
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10218716/
https://www.ncbi.nlm.nih.gov/pubmed/37240150
http://dx.doi.org/10.3390/ijms24108800
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