| Literature DB >> 33246101 |
Elee Shimshoni1, Idan Adir1, Ran Afik1, Inna Solomonov1, Anjana Shenoy2, Miri Adler3, Luca Puricelli4, Fabio Sabino5, Simonas Savickas5, Odelia Mouhadeb6, Nathan Gluck6, Sigal Fishman6, Lael Werner7, Tomer-Meir Salame8, Dror S Shouval7, Chen Varol6, Ulrich Auf dem Keller5, Alessandro Podestà4, Tamar Geiger2, Paolo Milani4, Uri Alon3, Irit Sagi9.
Abstract
Identification of early processes leading to complex tissue pathologies, such as inflammatory bowel diseases, poses a major scientific and clinical challenge that is imperative for improved diagnosis and treatment. Most studies of inflammation onset focus on cellular processes and signaling molecules, while overlooking the environment in which they take place, the continuously remodeled extracellular matrix. In this study, we used colitis models for investigating extracellular-matrix dynamics during disease onset, while treating the matrix as a complete and defined entity. Through the analysis of matrix structure, stiffness and composition, we unexpectedly revealed that even prior to the first clinical symptoms, the colon displays its own unique extracellular-matrix signature and found specific markers of clinical potential, which were also validated in human subjects. We also show that the emergence of this pre-symptomatic matrix is mediated by subclinical infiltration of immune cells bearing remodeling enzymes. Remarkably, whether the inflammation is chronic or acute, its matrix signature converges at pre-symptomatic states. We suggest that the existence of a pre-symptomatic extracellular-matrix is general and relevant to a wide range of diseases.Entities:
Keywords: Colitis; Electron microscopy; Extracellular matrix; Inflammation; Proteolysis; Proteomics
Year: 2020 PMID: 33246101 DOI: 10.1016/j.matbio.2020.11.001
Source DB: PubMed Journal: Matrix Biol ISSN: 0945-053X Impact factor: 11.583