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首页> 外文期刊>Journal of biomedical materials research, Part A >Immobilized sonic hedgehog N-terminal signaling domain enhances differentiation of bone marrow-derived mesenchymal stem cells
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Immobilized sonic hedgehog N-terminal signaling domain enhances differentiation of bone marrow-derived mesenchymal stem cells

机译:固定的刺猬N末端信号传导域增强了骨髓来源的间充质干细胞的分化

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摘要

The signaling domain of Sonic hedgehog (Shh), a potent upstream regulator of cell fate that has been implicated in osteoblast differentiation from undifferentiated mesenchymal cells in its endogenous form, was investigated in an immobilized form as a means for accelerating differentiation of uncommitted cells to the osteoblast phenotype. A recombinant cysteine-modified N-terminal Shh (mShh) was synthesized, purified, and immobilized onto interpenetrating polymer network (IPN) surfaces also grafted with a bone sialoprotein-derived peptide containing the Arg-Gly-Asp (RGD) sequence (bsp-RGD (15)), at calculated densities of 2.42 and 10 pmol/cm~2, respectively. The mitogenic effect of mShh was dependent on the mode of presentation, as surfaces with immobilized mShh and bsp-RGD (15) had no effect on the growth rate of rat bone marrow-derived mesenchymal stem cells (BMSCs), while soluble mShh enhanced cell growth compared to similar surface without mShh supplementation. In conjunction with media supplemented with bone morphogenetic pro tein-2 and -4, mShh and bsp-RGD (15)-grafted IPN surfaces enhanced the alkaline phosphatase activity of BMSCs compared with tissue culture polystyrene and bsp-RGD (15)-grafted IPN surfaces supplemented with soluble mShh, indicating enhanced osteoblast differentiation. The adhesive peptide bsp-RGD (15) was necessary for cell attachment and proliferation, as well as differentiation in response to immobilized mShh. The addition of immobilized Shh substantially improved the differentiation of uncommitted BMSCs to the osteoblast lineage, and therefore warrants further testing in vivo to examine the effect of the stated biomimetic system on peri-implant bone formation and implant fixation.
机译:Sonic刺猬(Shh)的信号传导域是一种细胞命运的有效上游调节剂,已以固定化形式研究了其以内源性形式从未分化的间充质细胞分化为成骨细胞的过程,以此作为加速未分化细胞向细胞分化的手段。成骨细胞表型。合成,纯化并固定了重组半胱氨酸修饰的N末端Shh(mShh)的互穿聚合物网络(IPN)表面,该表面也接枝了由唾液蛋白衍生的含有Arg-Gly-Asp(RGD)序列的肽(bsp- RGD(15)),计算密度分别为2.42和10 pmol / cm〜2。 mShh的促有丝分裂作用取决于呈递方式,因为固定有mShh和bsp-RGD的表面(15)对大鼠骨髓间充质干细胞(BMSCs)的生长速率没有影响,而可溶性mShh增强的细胞与不添加mShh的类似表面相比,生长快。与组织培养聚苯乙烯和bsp-RGD(15)移植的IPN相比,结合补充了骨形态发生蛋白2和-4的培养基,mShh和bsp-RGD(15)移植的IPN表面增强了BMSC的碱性磷酸酶活性。表面补充有可溶性mShh,表明成骨细胞分化增强。粘附肽bsp-RGD(15)对于细胞附着和增殖以及对固定的mShh的应答分化是必需的。固定化Shh的添加大大改善了未承诺BMSCs向成骨细胞谱系的分化,因此有必要在体内进行进一步测试,以检验所述仿生系统对植入物周围骨形成和植入物固定的影响。

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