4.8 Article

The role of simvastatin in the osteogenesis of injectable tissue-engineered bone based on human adipose-derived stromal cells and platelet-rich plasma

Journal

BIOMATERIALS
Volume 31, Issue 20, Pages 5325-5335

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.biomaterials.2010.03.037

Keywords

Simvastatin; Adipose-derived stromal cells; Platelet-rich plasma; Bone tissue engineering; Critical-sized calvarial defects; Injectable bone

Funding

  1. National Natural Science Foundation of China [30200319, 30901693]
  2. PKU school of stomatology for young scientists

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An injectable tissue-engineered bone (ITB) composed of human adipose-derived stromal cells (hADSCs) and platelet-rich plasma (hPRP) was preliminarily constructed, but its osteogenic capability needs improving. This study aimed to evaluate if simvastatin can be applied as a bone anabolic agent for this ITB. We found 0.01 mu m, 0.1 mu m, and 1 mu m simvastatin could induce hADSCs' osteoblastic differentiation in vitro that accompanied with non-inhibition on cell proliferation, high alkaline phosphatase activity, more mineralization deposition and more expression of osteoblast-related genes such as osteocalcin, core binding factor alpha 1, bone morphogenetic protein-2, vascular endothelial growth factor, and basic fibroblast growth factor. Simvastatin at 1 mu m seemed the most optimal concentration due to its high osteocalcin secretion in media (P < 0.01). Quantitative mineralization assay also showed 1 mu m SIM had the most obvious synergistic effect on hPRP's induction for matrix mineralization of hADSCs (P < 0.01). When 1 pm Simvastatin was applied to this ITB to restore the critical-sized calvarial defects in mice, more bone formation was observed in defected regions, and the peripheries just outside the defect margins by X-ray analysis, and H&E staining. These findings indicate that simvastatin at optimal concentrations can be used to promote this ITB's osteogenesis. However, simvastatin's effects on this ITB await long-term investigation. (C) 2010 Elsevier Ltd. All rights reserved.

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