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骨髓间充质基质细胞在骨源性支架上的成骨分化:微振动的影响及 ERK1/2 激活的作用。

Osteogenic differentiation of bone marrow-derived mesenchymal stromal cells on bone-derived scaffolds: effect of microvibration and role of ERK1/2 activation.

机构信息

State Key Laboratory of Oral Diseases, Sichuan University, Chengdu, 610041, P.R. China.

出版信息

Eur Cell Mater. 2011 Jul 6;22:12-25. doi: 10.22203/ecm.v022a02.

Abstract

Although in vivo studies have shown that low-magnitude, high-frequency (LMHF) vibration (LM: < 1 ×g; HF: 20-90 Hz) exhibits anabolic effects on skeletal homeostasis, the underlying cellular/molecular regulation involved in bone adaptation to LMHF vibration is little known. In this report, we tested the effects of microvibration (magnitude: 0.3 ×g, frequency: 40 Hz, amplitude: ± 50 μm, 30 min/12 h) on proliferation and osteodifferentiation of bone marrow-derived mesenchymal stromal cells (BMSCs) seeded on human bone-derived scaffolds. The scaffolds were prepared by partial demineralisation and deproteinisation. BMSCs were allowed to attach to the scaffolds for 3 days. Morphological study showed that spindle-shaped BMSCs almost completely covered the surface of bone-derived scaffold and these cells expressed higher ALP activity than those cultured on plates. After microvibration treatment, BMSC proliferation was decreased on day 7 and 10; however, numbers of genes and proteins expressed during osteogenesis, including Cbfa1, ALP, collagen I and osteocalcin were greatly increased. ERK1/2 activation was involved in microvibration-induced BMSC osteogenesis. Taken together, this study suggests that bone-derived scaffolds have good biocompatibility and show osteoinductive properties. By increasing the osteogenic lineage commitment of BMSCs and enhancing osteogenic gene expressions, microvibration promotes BMSC differentiation and increase bone formation of BMSCs seeded on bone-derived scaffolds. Moreover, ERK1/2 pathway plays an important role in microvibration-induced osteogenesis in BMSC cellular scaffolds.

摘要

尽管体内研究表明,低幅度、高频率(LM:<1×g;HF:20-90 Hz)的振动对骨骼稳态具有合成代谢作用,但骨对 LMHF 振动适应的潜在细胞/分子调节机制知之甚少。在本报告中,我们测试了微振动(幅度:0.3×g,频率:40 Hz,振幅:±50μm,30 分钟/12 小时)对骨髓间充质基质细胞(BMSCs)在人骨衍生支架上增殖和成骨分化的影响。支架通过部分脱矿质和脱蛋白化制备。BMSCs 被允许附着在支架上 3 天。形态学研究表明,纺锤形 BMSCs 几乎完全覆盖了骨衍生支架的表面,这些细胞的碱性磷酸酶(ALP)活性比在平板上培养的细胞更高。微振动处理后,第 7 天和第 10 天 BMSC 增殖减少;然而,成骨过程中表达的基因和蛋白数量(包括 Cbfa1、ALP、胶原 I 和骨钙素)大大增加。ERK1/2 激活参与了微振动诱导的 BMSC 成骨作用。综上所述,本研究表明骨衍生支架具有良好的生物相容性,并表现出成骨特性。通过增加 BMSCs 的成骨谱系分化,并增强成骨基因表达,微振动促进了 BMSCs 在骨衍生支架上的分化和增加了骨形成。此外,ERK1/2 通路在 BMSC 细胞支架中微振动诱导的成骨作用中发挥重要作用。

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