4.3 Article

Role of Adult Tissue-Derived Pluripotent Stem Cells in Bone Regeneration

Journal

STEM CELL REVIEWS AND REPORTS
Volume 16, Issue 1, Pages 198-211

Publisher

SPRINGER
DOI: 10.1007/s12015-019-09943-x

Keywords

VSEL; Stem cells; Bone healing; Critical size defect model; Osteoclastogenesis; In situ hybridization

Funding

  1. DFG [4922/3-1]
  2. Friedrichsheim Foundation (Stiftung Friedrichsheim) based in Frankfurt/Main, Germany

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BackgroundBone marrow-derived mononuclear cells (BM-MNC) consist of a heterogeneous mix of mesenchymal stem cells (MSC), hematopoietic progenitor cells (HPC), endothelial progenitor cells (EPC), monocytes, lymphocytes and pluripotent stem cells. Whereas the importance of MSC and EPC has been well documented in bone healing and regeneration studies, the role of pluripotent stem cells is still poorly understood. In the present study we evaluated if and how Very Small Embryonic Like cells (VSEL), isolated from rat BM-MNC, contribute to bone healing.MethodsLarge bone defects were made in the femurs of 38 Sprague Dawley female rats and treated with beta-TCP scaffold granules seeded with male VSEL; BM-MNC, VSEL-depleted BM-MNC or scaffold alone, and bone healing was evaluated at 8 weeks post-surgery.ResultsBone healing was significantly increased in defects treated with VSEL and BM-MNC, compared to defects treated with VSEL-depleted BM-MNC. Donor cells were detected in new bone tissue, in all the defects treated with cells, and in fibrous tissue only in defects treated with VSEL-depleted BM-MNC. The number of CD68+ cells was the highest in the VSEL-depleted group, whereas the number of TRAP positive cells was the lowest in this group.ConclusionsBased on the results, we can conclude that VSEL play a role in BM-MNC induced bone formation. In our rat femur defect model, in defects treated with VSEL-depleted BM-MNC, osteoclastogenesis and bone formation were decreased, and foreign body reaction was increased.

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