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Dynamics of Early Signalling Events during Fracture Healing and Potential Serum Biomarkers of Fracture Non-Union in Humans

机译:人类骨折愈合期间早期信号事件的动态及裂缝非联合骨折的潜在血清生物标志物

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To characterise the dynamic of events during the early phases of fracture repair in humans, we investigated molecular events using gene expression profiling of bone fragments from the fracture site at different time points after trauma and immune/stromal cells recruitment at the fracture site using flow cytometry. Bone and inflammatory markers were expressed at low levels at homeostasis, while transcripts for bone constituent proteins were consistently detected at higher levels. Early after fracture (range 2-4 days), increased expression of CXCL12, suggested recruitment of immune cells associated with a change in the balance of degradation enzymes and their inhibitors. At intermediate time after fracture (4-8 days), we observed high expression of inflammatory cytokines (IL1-beta, IL6), CCL2, the T-cell activation marker CD69. Late after fracture (8-14 days), high expression of factors co-operating towards the regulation of bone turnover was detected. We identified potential soluble factors and explored circulating levels in patients for whom a union/non-union (U/NU) outcome was known. This showed a clear difference for PlGF (p = 0.003) at day 1. These findings can inform future studies further investigating the cascade of molecular events following fractures and for the prediction of fracture non-union.
机译:为了表征在人类骨折修复早期阶段期间事件的动态,我们使用流式细胞术在裂缝部位在裂缝部位募集的不同时间点的骨折地区的骨片段中的基因表达分析研究了分子事件。骨骼和炎症标记物在稳态处的低水平表达,而在较高水平的骨构成蛋白的转录物始终检测到。在骨折(范围2-4天)后,CXCL12的表达增加,建议招募与降解酶及其抑制剂平衡的变化相关的免疫细胞。在骨折后的中间时间(4-8天),我们观察到炎性细胞因子(IL1-BETA,IL6),CCL2,T细胞活化标志物CD69的高表达。骨折后期(8-14天),检测到朝向调节骨质营业额的重点的高表达。我们确定了潜在的可溶解因子,并探讨了联合/非联盟(U / NU)结果的患者中的循环水平。这对第1天的PLGF(P = 0.003)显示了明显的差异。这些发现可以通知未来的研究进一步研究骨折后裂缝后的分子事件的级联和预测骨折非联盟。

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