Résumé
In osteoarthritis (OA), articular chondrocytes display phenotypic and functional changes associated with epigenomic alterations. These changes contribute to the disease progression, which is characterized by dysregulated reparative processes and abnormal extracellular matrix remodeling leading to cartilage degradation. Recent studies using a murine model of posttraumatic OA highlighted the contribution of changes in DNA hydroxymethylation (5hmC) to OA progression. Here, we integrated transcriptomic and epigenomic analyses in cartilage after induction of OA to show that the structural progression of OA is accompanied by early transcriptomic and pronounced DNA methylation (5mC) changes in chondrocytes. These changes accumulate over time and are associated with recapitulation of developmental processes, including cartilage development, chondrocyte hypertrophy, and ossification. Our integrative analyses also uncovered that Lrrc15 is differentially methylated and expressed in OA cartilage, and that it may contribute to the functional and phenotypic alterations of chondrocytes, likely coordinating stress responses and dysregulated extracellular matrix remodeling.
| Langue d'origine | English |
|---|---|
| Numéro d'article | 21107 |
| Journal | Scientific Reports |
| Volume | 11 |
| Numéro de publication | 1 |
| DOI | |
| Statut de publication | Published - déc. 2021 |
Financement
This work was supported by National Institutes of Health Grant R21 AG049980 (M.O.). M.W. received support from a Scholarship from the Xi’an Jiaotong University. The authors are also grateful to the Tow Foundation, which provided support for the David Z. Rosensweig Genomics Research Center, Giammaria Giuliani, Marina Kellen French and the Anna-Maria and Stephen Kellen French Foundation, the Ira W. DeCamp Foundation, and the Ambrose Monell Foundation. This work was supported by National Institutes of Health Grant R21 AG049980 (M.O.). M.W. received support from a Scholarship from the Xi’an Jiaotong University. The authors are also grateful to the Tow Foundation, which provided support for the David Z. Rosensweig Genomics Research Center, Giammaria Giuliani, Marina Kellen French and the Anna-Maria and Stephen Kellen French Foundation, the Ira W. DeCamp Foundation, and the Ambrose Monell Foundation. Technical support was provided by the Epigenomics Core of Weill Cornell Medicine, and the HSS Research Institute Histopathology Service. The authors are thankful to Ms. Orla O’Shea for her help with the LRRC15 immunostaining, and to Dr. Carl Blobel’s laboratory for their help with the LRRC15 immunoblotting.
| Bailleurs de fonds | Numéro du bailleur de fonds |
|---|---|
| HSS Research Institute Histopathology Service | |
| Stephen Kellen French Foundation | |
| National Institutes of Health | |
| National Institute on Aging | R21AG049980 |
| Ambrose Monell Foundation | |
| Ira W. DeCamp Foundation | |
| Tow Foundation | |
| Xi’an Jiaotong University |
ASJC Scopus Subject Areas
- General