首页> 美国卫生研究院文献>International Journal of Clinical and Experimental Pathology >Systemic BMSC homing in the regeneration of pulp-like tissue and the enhancing effect of stromal cell-derived factor-1 on BMSC homing
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Systemic BMSC homing in the regeneration of pulp-like tissue and the enhancing effect of stromal cell-derived factor-1 on BMSC homing

机译:牙髓样组织再生中的全身BMSC归巢和基质细胞衍生因子1对BMSC归巢的增强作用

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摘要

Pulp regeneration caused by endogenous cells homing has become the new research spot in endodontics. However, the source of functional cells that are involved in and contributed to the reconstituting process has not been identified. In this study, the possible role of systemical BMSC in pulp regeneration and the effect of stromal cell-derived factor-1 (SDF-1) on stem cell recruitment and angiogenesis were evaluated. 54 mice were divided into three groups: SDF-1 group (subcutaneous pockets containing roots with SDF-1 absorbed neutralized collagen gel and the green fluorescent protein (GFP) positive BMSCs transplantation via the tail vein), SDF-1-free group (pockets containing roots with gel alone and GFP + BMSCs transplantation) and Control group (pockets containing roots with gel alone). The animals were sacrificed after the roots were implanted into subcutaneous pockets for 3 weeks. Histomorphometric analysis was performed to evaluate the regenerated tissue in the canal by hematoxylin and eosin (HE) staining. The homing of the transplanted BMSCs was monitored with a fluorescence microscope and immunohistochemical analysis. The expression of ALP in new formed tissue was detected immunohistochemically. Dental-pulp-like tissue and new vessels were regenerated and GFP-positive BMSCs and expression of ALP could be observed in both SDF-1 group and SDF-1-free group. Furthermore, more GFP+ cells, stronger expression of ALP and stronger angiogenesis were found in the SDF-1 group than in the SDF-1-free group. To conclude, systemic BMSC can home to the root canal and participate in dental-pulp-like tissue regeneration. Intracanal application of SDF-1 may enhance BMSC homing efficiency and angiogenesis.
机译:由内源性细胞归巢引起的牙髓再生已成为牙髓治疗的新研究热点。但是,尚未发现参与重组过程并对其起作用的功能性细胞来源。在这项研究中,评估了系统性BMSC在牙髓再生中的可能作用以及基质细胞衍生因子1(SDF-1)对干细胞募集和血管生成的影响。 54只小鼠分为三组:SDF-1组(皮下囊袋,其根部带有SDF-1吸收的中和胶原凝胶和绿色荧光蛋白(GFP)通过尾静脉移植的阳性BMSCs),无SDF-1的组(囊袋)含有单独凝胶的根和GFP + BMSCs移植)和对照组(含有单独凝胶的根的口袋)。将根植入皮下口袋3周后处死动物。进行组织形态计量学分析以通过苏木精和曙红(HE)染色评估管中的再生组织。用荧光显微镜和免疫组织化学分析监测移植的BMSC的归巢。免疫组织化学检测ALP在新形成的组织中的表达。牙髓样组织和新血管再生,在SDF-1组和无SDF-1组中均可观察到GFP阳性的BMSC和ALP的表达。此外,与不含SDF-1的组相比,在SDF-1组中发现更多的GFP +细胞,更强的ALP表达和更强的血管生成。总之,全身性BMSC可以回到根管并参与牙髓样组织的再生。 SDF-1的腔内应用可增强BMSC归巢效率和血管生成。

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