4.6 Article

Anti-hypertrophic effect of synovium-derived stromal cells on costal chondrocytes promotes cartilage repairs

期刊

JOURNAL OF ORTHOPAEDIC TRANSLATION
卷 32, 期 -, 页码 59-68

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ELSEVIER
DOI: 10.1016/j.jot.2021.05.002

关键词

Costal chondrocyte; Synovium-derived mesenchymal stromal cell; Hypertrophic differentiation

资金

  1. National Natural Science Foundation of China [81820108020]
  2. Innovative Research Team of High-Level Local Universities in Shanghai [SSMU-ZDCX20180800]

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This study demonstrates that synovium-derived stromal cells (SDSCs) can help coastal chondrocytes (CCs) maintain their chondrogenic phenotype and suppress hypertrophic differentiation in cartilage repairs through both direct and indirect coculture experiments. The presence of SDSCs in osteochondral defects promotes good restoration effects and lower expression levels of type X collagen, suggesting a potential role for SDSCs in cartilage repair.
Background: Costal chondrocytes (CCs), as a promising donor cell source for cell-based therapy for cartilage repair, have strong tendency of hypertrophy and calcification, which limited CCs from further application in cartilage regenerative medicine. Synovium-derived stromal cells (SDSCs), have shown their beneficial effect for chondrocytes to maintain phenotype. This study aims to investigate whether SDSCs could help CCs to maintain chondrogenic phenotype and suppress hypertrophic differentiation in cartilage repairs. Methods: CCs were directly cocultured with SDSCs in pellet or indirectly cocultured using a conditioned medium in vitro for 3 weeks. Cartilage matrix formation and hypertrophic differentiation of CCs were analyzed by RT-PCR, biochemical assays, and histological staining. Cocultured pellets were implanted into the osteochondral defects made on the femoral groove of the rats. Then, macroscopic and histological evaluations were performed. Results: Pellets formed by CCs alone and CCs cocultured with SDSCs reveal equal cartilage matrix deposition. However, the gene expression of type X collagen was significantly downregulated in cocultured pellets. Immunohistochemistry analysis revealed suppressed expression of type X collagen in cocultured pellets, indicating SDSCs may suppress hypertrophic differentiation of chondrocytes. Further in indirect coculture experiment, SDSCs suppressed type X collagen expression as well and promoted the proliferation of CCs, indicating SDSCs may influence CCs by paracrine mechanism. The pellets implanted in the osteochondral defects showed good restoration effects, whereas the grafts constructed with CCs and SDSCs showed lower type X expression levels. Conclusion These results suggest that SDSCs may maintain the phenotype of CCs and prevent the hypertrophic differentiation of CCs in cartilage repair.

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