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Osteogenic Differentiation of Human Mesenchymal Bone Marrow Cells in Silk Scaffolds Is Regulated by Nitric Oxide

机译:丝支架中人间充质骨髓细胞的骨质发生分化由一氧化氮调节

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Bone marrow-derived mesenchymal stem cells (BMSC) are a powerful tool for tissue engineering and can be used in the regeneration of bone and other tissues. Nitric oxide (NO) produced by the endothelial NO synthase (eNOS) plays an important role in bone development and healing. We hypothesized that NO plays a role in osteogenic differentiation of BMSC cultured in three-dimensional silk scaffolds. eNOS protein was measured by Western Analysis and its activity was assessed by measuring nitrite in culture supernatants. Mineralization was evaluated through calcium deposition and the expression of genes associated with osteogenic differentiation (collagen I, RUNX2, and osteocalcin) was quantified using real-time RT-PCR. eNOS was consistently expressed with minor fluctuations, but NO production significantly increased at later time points (weeks 4 and 5). Addition of a competitive NOS inhibitor (LNAME) resulted in a modest decrease in calcium deposition, which became statistically significant in week 5. This was preceded by a dramatic decrease in RUNX2 and osteocalcin expression in week 4. These results support our hypothesis and implicate NO as an important player in bone tissue engineering.
机译:骨髓衍生的间充质干细胞(BMSC)是组织工程的强大工具,可用于骨骼和其他组织的再生。通过内皮没有合成酶(Enos)产生的一氧化氮(NO)在骨发育和愈合中起着重要作用。我们假设不发挥在三维丝支架中培养的BMSC的成骨分化中的作用。通过西方分析测量eNOS蛋白,通过在培养上清液中测量亚硝酸盐来评估其活性。通过钙沉积评价矿化,并使用实时RT-PCR定量与骨质发生分化(胶原蛋白I,Runx2和Osteocalcin)相关的基因的表达。 ENOS始终用轻微的波动表达,但在稍后的时间点(第4周和第5周)没有生产明显增加。添加具有竞争性的NoS抑制剂(LNAME)导致钙沉积的温度下降,这在第5周变得统计学意义。这是在第4周内润X2和骨钙素表达的急剧下降。这些结果支持我们的假设并牵连作为骨组织工程的重要球员。

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