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首页> 外文期刊>Journal of the Serbian Chemical Society >Antiosteogenic effect of arsenic trioxide, cholecalciferol, lovastatin or their combination in vitro
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Antiosteogenic effect of arsenic trioxide, cholecalciferol, lovastatin or their combination in vitro

机译:三氧化二砷,胆钙化固醇,洛伐他汀或其组合的体外抗骨形成作用

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Pathological formation of bone in non-skeletal soft tissues or heterotopic ossification (HO), for which there is currently no effective treatment, is considered to be mediated by activation of Hedgehog (Hh) signaling pathway. Moreover, the biochemical mechanism of this pathological process is not fully understood. Here, we tested the efficacy of three chemical inhibitors of the Hh signaling pathway, arsenic trioxide (ATO), lovastatin (Lov) and cholecalciferol (Vitamin D) to hamper differentiation of mesenchymal stem cells (MSC) into osteoblasts or osteogenesis. Each of the three Hh inhibitors potently decreased alkaline phosphatase activity, suggesting effective suppression of osteogenic activity in Hh-impaired MSC. Gene expression analysis revealed a significant reduction in mRNA levels of chief Hh signaling marker, Gli1, following administration of Hh small molecule inhibitors. A functional link between Hedgehog and osteogenesis in native MSC cells is further established in studies involving the mix of three Hh inhibitors acting at different checkpoints of the Hh signaling pathway. Thus, a combination of small molecule inhibitors of the Hh pathway at their lower concentrations could be a novel approach for HO prophylaxis with increased efficacy and potentially reduced side effects.
机译:目前尚无有效治疗方法的非骨骼软组织中的骨病理形成或异位骨化(HO)被认为是由Hedgehog(Hh)信号通路的激活介导的。而且,这种病理过程的生化机理还没有被完全理解。在这里,我们测试了Hh信号传导途径的三种化学抑制剂三氧化二砷(ATO),洛伐他汀(Lov)和胆钙化固醇(维生素D)抑制间充质干细胞(MSC)分化为成骨细胞或成骨的功效。三种Hh抑制剂均会有效降低碱性磷酸酶的活性,表明在Hh受损的MSC中有效抑制了成骨活性。基因表达分析显示,施用Hh小分子抑制剂后,主要Hh信号标记Gli1的mRNA水平显着降低。在涉及在Hh信号传导途径的不同检查点起作用的三种Hh抑制剂的混合物的研究中,进一步建立了天然MSC细胞中刺猬与成骨之间的功能联系。因此,以较低的浓度组合Hh途径的小分子抑制剂可能是一种预防HO的新方法,具有更高的疗效和潜在的副作用。

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