首页> 美国卫生研究院文献>European Journal of Histochemistry : EJH >Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporation
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Analysis of mineral apposition rates during alveolar bone regeneration over three weeks following transfer of BMP-2/7 gene via in vivo electroporation

机译:通过体内电穿孔转移BMP-2 / 7基因后三周内牙槽骨再生过程中矿物质沉积速率的分析

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摘要

Alveolar bone is not spontaneously regenerated following trauma or periodontitis. We previously proposed an animal model for new alveolar bone regeneration therapy based on the non-viral BMP-2/7 gene expression vector and in vivo electroporation, which induced the formation of new alveolar bone over the course of a week. Here, we analysed alveolar bone during a period of three weeks following gene transfer to periodontal tissue. Non-viral plasmid vector pCAGGS-BMP-2/7 or pCAGGS control was injected into palatal periodontal tissue of the first molar of the rat maxilla and immediately electroporated with 32 pulses of 50 V for 50 msec. Over the following three weeks, rats were double bone-stained by calcein and tetracycline every three days and mineral apposition rates (MAR) were measured. Double bonestaining revealed that MAR of alveolar bone was at similar level three days before BMP-2/7 gene transfer as three days after gene transfer. However, from 3 to 6 days, 6 to 9 days, 9 to 12 days, 12 to 15 days, 15 to 18 days, and 18 to 20 days after, MARs were significantly higher than prior to gene transfer. Our proposed gene therapy for alveolar bone regeneration combining nonviral BMP-2/7 gene expression vector and in vivo electroporation could increase alveolar bone regeneration potential in the targeted area for up to three weeks.
机译:创伤或牙周炎后,牙槽骨不会自发再生。我们先前基于非病毒BMP-2 / 7基因表达载体和体内电穿孔,提出了一种用于新牙槽骨再生治疗的动物模型,该模型在一周的时间内诱导了新牙槽骨的形成。在这里,我们分析了基因转移到牙周组织后三周内的牙槽骨。将非病毒质粒载体pCAGGS-BMP-2 / 7或pCAGGS对照注射到大鼠上颌第一磨牙的pa牙周组织中,并立即用32个50 V脉冲电穿孔50毫秒。在接下来的三周中,每三天对大鼠进行钙黄绿素和四环素双染,并测量矿物质的沉积率(MAR)。双骨染色显示,在BMP-2 / 7基因转移前三天,牙槽骨的MAR与基因转移后三天处于相似的水平。然而,在3至6天,6至9天,9至12天,12至15天,15至18天以及18至20天之后,MAR明显高于基因转移之前。我们提出的结合非病毒BMP-2 / 7基因表达载体和体内电穿孔的牙槽骨再生基因治疗可以在目标区域最多增加三周的牙槽骨再生潜力。

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