胰岛素样生长因子-1 和血小板衍生生长因子-α对人脂肪来源的基质细胞成骨分化的调节。
Regulation of human adipose-derived stromal cell osteogenic differentiation by insulin-like growth factor-1 and platelet-derived growth factor-alpha.
机构信息
Stanford, Calif. From the Hagey Pediatric Regenerative Research Laboratory, Department of Surgery, Plastic and Reconstructive Surgery Division, Stanford University School of Medicine.
出版信息
Plast Reconstr Surg. 2010 Jul;126(1):41-52. doi: 10.1097/PRS.0b013e3181da8858.
BACKGROUND
Human adipose-derived stromal cells possess a great potential for tissue engineering purposes. The authors' laboratory is interested in harnessing human adipose-derived stromal cells for skeletal tissue regeneration and identifying those factors that enhance human adipose-derived stromal cell osteogenic differentiation. The authors hypothesized that insulin-like growth factor (IGF) and platelet-derived growth factor (PDGF) would stimulate human adipose-derived stromal cell osteogenesis and that IGF would stimulate adipogenesis.
METHODS
Adipose-derived stromal cells were harvested from human lipoaspirate. Previously, a microarray analysis examined gene expression throughout osteogenic differentiation. In a candidate fashion, the authors added recombinant IGF-1 and PDGF-alpha individually and in combination. Osteogenesis and adipogenesis were assessed by alkaline phosphatase, alizarin red, and oil red O staining, and quantitative real-time polymerase chain reaction (RUNX2, ALP, OCN, IGF1, PPARG, LPL, AP2, and GCP1). Finally, intersection between IGF and PDGF signaling pathways was evaluated.
RESULTS
IGF-1 was observed to increase osteogenic differentiation by all markers (p < 0.01). However, PDGF-alpha when added alone primarily did not affect osteogenic markers. PDGF-alpha positively regulated transcription of IGF1. Addition of PDGF-alpha in combination with or before IGF-1 enhanced osteogenesis more than either alone. IGF-1 increased whereas PDGF-alpha diminished human adipose-derived stromal cell adipogenesis.
CONCLUSIONS
IGF signaling significantly increased osteogenesis in human adipose-derived stromal cells and may be used for tissue-engineering purposes. The combination of PDGF and IGF may be more beneficial than either alone in driving adipose-derived stromal cell osteogenesis. Future in vivo applications will focus on the combination of adipose-derived stromal cells, biomimetic scaffolds, and recombinant IGF.
背景
人类脂肪来源的基质细胞在组织工程中有很大的潜力。作者实验室有兴趣利用人类脂肪来源的基质细胞进行骨骼组织再生,并确定那些能增强人类脂肪来源的基质细胞成骨分化的因素。作者假设胰岛素样生长因子(IGF)和血小板衍生生长因子(PDGF)将刺激人类脂肪来源的基质细胞成骨,并刺激 IGF 脂肪生成。
方法
从人体脂肪抽吸物中收获脂肪来源的基质细胞。之前,微阵列分析检查了整个成骨分化过程中的基因表达。作者以候选方式单独和组合添加重组 IGF-1 和 PDGF-α。通过碱性磷酸酶、茜素红和油红 O 染色以及定量实时聚合酶链反应(RUNX2、ALP、OCN、IGF1、PPARG、LPL、AP2 和 GCP1)评估成骨和脂肪生成。最后,评估了 IGF 和 PDGF 信号通路的交叉。
结果
IGF-1 被观察到通过所有标志物增加成骨分化(p<0.01)。然而,单独添加 PDGF-α 主要不会影响成骨标志物。PDGF-α 正向调节 IGF1 的转录。与单独添加 IGF-1 相比,添加 PDGF-α 组合或之前会增强成骨作用。IGF-1 增加,而 PDGF-α 减少人类脂肪来源的基质细胞脂肪生成。
结论
IGF 信号显著增加了人类脂肪来源的基质细胞的成骨作用,可用于组织工程目的。PDGF 和 IGF 的组合可能比单独使用任何一种都更有利于驱动脂肪来源的基质细胞成骨作用。未来的体内应用将集中在脂肪来源的基质细胞、仿生支架和重组 IGF 的组合上。
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