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首页> 外文期刊>Frontiers in Bioengineering and Biotechnology >Five Days Granulocyte Colony-Stimulating Factor Treatment Increases Bone Formation and Reduces Gap Size of a Rat Segmental Bone Defect: A Pilot Study
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Five Days Granulocyte Colony-Stimulating Factor Treatment Increases Bone Formation and Reduces Gap Size of a Rat Segmental Bone Defect: A Pilot Study

机译:五天粒细胞集落刺激因子治疗可增加大鼠节段性骨缺损的骨形成并缩小间隙大小:一项先导研究

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Bone is an organ with high natural regenerative capacity and most fractures heal spontaneously when appropriate fracture fixation is provided. However, additional treatment is required for patients with large segmental defects exceeding the endogenous healing potential and for patients suffering from fracture non-unions. These cases are often associated with insufficient vascularization. Transplantation of CD34+ endothelial progenitor cells (EPCs) has been successfully applied to promote neovascularization of bone defects, however including extensive ex vivo manipulation of cells. Here we hypothesized, that treatment with Granulocyte colony-stimulating factor (G-CSF) may improve bone healing by mobilization of CD34+ progenitor cells into the circulation, which in turn may facilitate vascularization at the defect site. In this pilot study, we aimed to characterize the different cell populations mobilized by G-CSF and investigate the influence of cell mobilization on the healing of a critical size femoral defect in rats. Cell mobilization was investigated by flow cytometry at different time points after five consecutive daily G-CSF injections. In a pilot study, bone healing of a 4.5 mm critically-sized femoral defect in F344 rats was compared between a saline-treated control group and a G-CSF treatment group. In vivo micro computed tomography and histology were applied to compare bone formation in both treatment groups. Our data revealed that leukocyte counts show a peak increase at the first day after the last G-CSF injection. In addition, we found that CD34+ progenitor cells, including EPCs, were significantly enriched at day 1, and further increased at day 5 and day 11. Upregulation of monocytes, granulocytes and macrophages peaked at day 1. G-CSF treatment significantly increased bone volume and bone density in the defect, which was confirmed by histology. Our data show that different cell populations are mobilized by G-CSF treatment in cell specific patterns. Although in this pilot study no bridging of the critically-sized defect was observed, significantly improved bone formation by G-CSF treatment was clearly shown.
机译:骨是具有高自然再生能力的器官,只要提供适当的骨折固定,大多数骨折都会自愈。但是,对于节段性缺陷超过内源性愈合潜能的患者以及骨折不愈合的患者,需要额外的治疗。这些情况通常与血管生成不足有关。 CD34 +内皮祖细胞(EPC)的移植已成功应用于促进骨缺损的新生血管形成,但包括对细胞的广泛离体操作。在这里我们假设,粒细胞集落刺激因子(G-CSF)的治疗可通过动员CD34 +祖细胞进入循环系统来改善骨愈合,进而促进缺损部位的血管形成。在这项前期研究中,我们旨在表征由G-CSF动员的不同细胞群体,并研究细胞动员对大鼠临界股骨缺损愈合的影响。连续五天每天注射G-CSF后,在不同时间通过流式细胞仪研究细胞动员。在一项先导研究中,比较了用盐水治疗的对照组和G-CSF治疗组的F344大鼠中4.5 mm临界尺寸的股骨缺损的骨愈合情况。应用体内计算机断层扫描和组织学比较两个治疗组的骨形成。我们的数据显示,白细胞计数显示在最后一次G-CSF注射后的第一天出现峰值增加。此外,我们发现CD34 +祖细胞(包括EPC)在第1天显着富集,并在第5天和第11天进一步增加。单核细胞,粒细胞和巨噬细胞的上调在第1天达到峰值。G-CSF治疗显着增加了骨体积组织学证实了缺损的骨密度。我们的数据表明,通过G-CSF处理以特定于细胞的模式动员了不同的细胞群。尽管在该初步研究中未观察到临界尺寸缺损的桥接,但仍清楚显示了通过G-CSF治疗可显着改善骨形成。

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