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Effect of Alendronate on Bone Formation during Tooth Extraction Wound Healing

机译:阿仑膦酸钠对拔牙创面愈合过程中骨形成的影响

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摘要

Alendronate (ALN) is an antiresorptive agent widely used for the treatment of osteoporosis. Its suppressive effect on osteoclasts has been extensively studied. However, the effect of ALN on bone formation is not as clear as its effect on resorption. The objective was to determine the effect of short-term ALN on bone formation and tooth extraction wound healing. Molar tooth extractions were performed in mice. ALN, parathyroid hormone (PTH), or saline (vehicle control) was administered. PTH was used as the bone anabolic control. Mice were euthanized at 3, 5, 7, 10, and 21 d after extractions. Hard tissue healing was determined histomorphometrically. Neutrophils and lymphatic and blood vessels were quantified to evaluate soft tissue healing. Gene expression in the wounds was assessed at the RNA level. Furthermore, the vossicle bone transplant system was used to verify findings from extraction wound analysis. Alkaline phosphatase (ALP) was visualized in the vossicles to assess osteoblast activity. ALN exhibited no negative effect on bone formation. In intact tibiae, ALN increased bone mass significantly more than PTH did. Consistently, significantly elevated osteoblast numbers were noted. In the extraction sockets, bone fill in the ALN-treated mice was equivalent to the control. Genes associated with bone morphogenetic protein signaling, such as bmp2, nog, and dlx5, were activated in the extraction wounds of the ALN-treated animals. Bone formation in vossicles was significantly enhanced in the ALN versus PTH group. In agreement with this, ALN upregulated ALP activity considerably in vossicles. Neutrophil aggregation and suppressed lymphangiogenesis were evident in the soft tissue at 21 d after extraction, although gross healing of extraction wounds was uneventful. Bone formation was not impeded by short-term ALN treatment. Rather, short-term ALN treatment enhanced bone formation. ALN did not alter bone fill in extraction sockets.
机译:阿仑膦酸酯(ALN)是一种抗吸收剂,广泛用于治疗骨质疏松症。已经广泛研究了其对破骨细胞的抑制作用。然而,ALN对骨形成的影响不如其对吸收的影响那么明显。目的是确定短期ALN对骨形成和拔牙创面愈合的影响。在小鼠中进行臼齿拔牙。给予ALN,甲状旁腺激素(PTH)或生理盐水(车辆对照)。 PTH被用作骨合成代谢对照。提取后第3、5、7、10和21天对小鼠实施安乐死。硬组织愈合通过组织形态学测定。嗜中性粒细胞和淋巴管及血管被量化以评估软组织的愈合。在RNA水平评估伤口中的基因表达。此外,小囊骨移植系统用于验证提取伤口分析的结果。在小泡中观察碱性磷酸酶(ALP),以评估成骨细胞的活性。 ALN对骨形成没有负面影响。在完整的胫骨中,ALN的骨质增加明显超过PTH。一致地,注意到成骨细胞数量显着升高。在拔牙窝中,经ALN处理的小鼠的骨填充量与对照组相当。与骨形态发生蛋白信号传导相关的基因,例如bmp2,nog和dlx5,在经ALN处理的动物的提取伤口中被激活。与PTH组相比,ALN的小囊骨形成明显增强。与此相符,ALN在小泡中显着上调了ALP活性。拔牙后21 d,软组织中嗜中性粒细胞聚集和抑制的淋巴管生成明显,尽管拔牙伤口的总体愈合良好。短期ALN治疗不会阻止骨形成。相反,短期ALN治疗可增强骨形成。 ALN不会改变拔牙窝中的骨填充。

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