Portal de investigación
Resistance to apoptosis in complicated Crohn's disease: Relevance in ileal fibrosis
Fecha de publicación:
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Autores de INCLIVA
Participantes ajenos a INCLIVA
- Ortiz-Masiá, D
- Macias-Ceja, DC
- Coll, S
- Gisbert-Ferrándiz, L
- Cósin-Roger, J
- Bauset, C
- Ortega, M
- Navarro-Vicente, F
- Millan, M
- Esplugues, JV
- Calatayud, S
- Barrachina, MD
Grupos y Plataformas de I+D+i
Abstract
Background and aims: The stiffening of the extracellular matrix, and changes in its cellular and molecular composition, have been reported in the pathogenesis of fibrosis. We analyze the mechanisms that perpetuate ileal fibrosis in surgical resections of complicated Crohn's disease patients.Methods: Ileal resections were obtained from affected and non-affected tissue of stenotic or penetrating Crohn's disease behavior. Ilea from non-IBD patients were used as control tissue. All samples underwent RNA sequencing. Human small intestinal fibroblasts were treated for 48 h with IL-1 beta, TFG beta 1, PDGFB or TNF-alpha. Resistance to apoptosis was analysed by RT-PCR, western blot and immunohistochemistry in ileal tissue and by RT-PCR and FACS in cultured cells.Results: Growth factor-driven signaling pathways and increased RAS GTPase activity were up-regulated in affected ilea in which we found expression of both the antiapoptotic molecule MCL1 and the transcription factor ETS1 in submucosal fibroblasts, and a senescence-associated secretory phenotype. In cultured intestinal fibro-blasts, PDGFB induced an ETS1-mediated resistance to apoptosis that was associated with the induction of both of TGFB1 and IL1B, a cytokine that replicated the expression of SASP detected in ileal tissue. ETS1 drove fibroblast polarization between inflammatory and fibrogenic phenotypes in IL1 beta-treated cells. Conclusions: Our data show resistance to apoptosis in complicated ileal CD, and demonstrate that PDGFB induce an ETS1-mediated resistance to apoptosis associated with an inflammatory and fibrogenic pattern of expression in intestinal fibroblasts. Results point to PDGFRB, IL1R1 or MCL1 as potential targets against ileal fibrosis.
Copyright © 2023 The Authors. Published by Elsevier B.V. All rights reserved.
Datos de la publicación
- ISSN/ISSNe:
- 0925-4439, 1879-260X
- Tipo:
- Article
- Páginas:
- 166966-166966
- PubMed:
- 37995775
BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR BASIS OF DISEASE ELSEVIER SCIENCE BV
Citas Recibidas en Web of Science: 3
Documentos
- No hay documentos
Filiaciones
Keywords
- Fibrosis; Crohn's disease; Fibroblasts; Apoptosis; Senescence -associated secretory phenotype
Financiación
Cita
Resistance to apoptosis in complicated Crohn's disease: Relevance in ileal fibrosis. Seco M, Ortiz D, Macias DC, Coll S, Gisbert L, Cósin J, Bauset C et al. BIOCHIMICA ET BIOPHYSICA ACTA-MOLECULAR BASIS OF DISEASE. 2024 febrero 01. 1870 (2):166966-166966. DOI:10.1016/j.bbadis.2023.166966. PMID:37995775.
