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doi: 10.1111/jcmm.14283
pmid: 30903650
pmc: PMC6533528
handle: 2183/23318 , 20.500.14352/13485 , 20.500.11940/15942 , 10261/241509 , 20.500.12530/64433
doi: 10.1111/jcmm.14283
pmid: 30903650
pmc: PMC6533528
handle: 2183/23318 , 20.500.14352/13485 , 20.500.11940/15942 , 10261/241509 , 20.500.12530/64433
AbstractFailure of therapeutic approaches for the treatment of osteoarthritis (OA) based on the inhibition of metalloproteinases, might be because of their constitutive expression in homeostasis, together with their network complexity. The knowledge of this network would contribute to selective target pathological conditions. In this sense, blockade of mediators produced by neighbouring joint cells, such as synovial fibroblasts (SF), would prevent cartilage damage. Thus, we studied the contribution of ADAMTS‐7 and ‐12 from SF to cartilage oligomeric matrix protein (COMP) degradation, and the signalling pathways involved in their expression. We report for the first time in SF, the involvement of ERK‐Runx2 axis and Wnt/β‐catenin signalling in ADAMTS‐12 and ADAMTS‐7 expressions, respectively, with the subsequent consequences in COMP degradation from cartilage extracellular matrix. After stimulation with IL‐1β or fibronectin fragments, we showed that ERK inhibition decreased Runx2 activation and ADAMTS‐12 expression in OA‐SF, also reducing Fn‐fs‐induced COMP degradation. Blockage of Wnt signalling by DKK1 reduced ADAMTS‐7 and COMP degradation in OA‐SF as well. In addition, Wnt7B expression was induced by IL‐1β and by itself, also increasing ADAMTS‐7. Our results could contribute to the development of disease‐modifying OA drugs targeting ADAMTS‐7 and ‐12 for the prevention of extracellular matrix components degradation like COMP.
Male, humanos, Interleukin-1beta, Bioquímica (Biología), Core Binding Factor Alpha 1 Subunit, Cartilage Oligomeric Matrix Protein, 3205.09 Reumatología, ADAMTS Proteins, ADAMTS-12, Runx2, ADAMTS-7, 616.72-002, Wnt Signaling Pathway, Wnt signalling, anciano, 577.112.6, ADAMTS‐7, Synovial Membrane, Extracellular matrix, proteína oligomérica de la matriz del cartílago, Reumatología, subunidad alfa 1 del factor de unión central, Extracellular Matrix, membrana sinovial, synovial fibroblasts, INIBIC, Female, Bioquímica, ADAMTS‐12, extracellular matrix, fibronectinas, ADAMTS7 Protein, interleucina-1beta, CHUAC, matriz extracelular, vía de señalización Wnt, Runx2 synovial fibroblasts, 2302 Bioquímica, Osteoarthritis, Humans, Synovial fibroblasts, Aged, Wnt signalling fibroblasts, COMP, Original Articles, Fibroblasts, Fibronectins, osteoarthritis, osteoartritis, fibroblastos, cartílago, Cartilage
Male, humanos, Interleukin-1beta, Bioquímica (Biología), Core Binding Factor Alpha 1 Subunit, Cartilage Oligomeric Matrix Protein, 3205.09 Reumatología, ADAMTS Proteins, ADAMTS-12, Runx2, ADAMTS-7, 616.72-002, Wnt Signaling Pathway, Wnt signalling, anciano, 577.112.6, ADAMTS‐7, Synovial Membrane, Extracellular matrix, proteína oligomérica de la matriz del cartílago, Reumatología, subunidad alfa 1 del factor de unión central, Extracellular Matrix, membrana sinovial, synovial fibroblasts, INIBIC, Female, Bioquímica, ADAMTS‐12, extracellular matrix, fibronectinas, ADAMTS7 Protein, interleucina-1beta, CHUAC, matriz extracelular, vía de señalización Wnt, Runx2 synovial fibroblasts, 2302 Bioquímica, Osteoarthritis, Humans, Synovial fibroblasts, Aged, Wnt signalling fibroblasts, COMP, Original Articles, Fibroblasts, Fibronectins, osteoarthritis, osteoartritis, fibroblastos, cartílago, Cartilage
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