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未成熟和成熟恒牙牙本质-牙髓复合体中的血管形成及VEGF/VEGFR2信号传导

Vascularity and VEGF/VEGFR2 Signaling in the Dentine-Pulp Complex of Immature and Mature Permanent Teeth.

作者信息

Friedlander Lara T, Coates Dawn, Seymour Gregory, Cullinan Mary, Rich Alison M

机构信息

Department of Oral Rehabilitation, Sir John Walsh Research Institute, Faculty of Dentistry, University of Otago, New Zealand.

Department of Oral Diagnostic and Surgical Sciences, University of Queensland, Brisbane, Australia.

出版信息

Eur Endod J. 2018 Nov 21;3(3):153-159. doi: 10.14744/eej.2018.07269. eCollection 2018.

Abstract

OBJECTIVE

To examine the microvessel density (MVD) and spatial distribution of endothelial cells and angiogenic activity in immature and mature permanent teeth using immunohistochemistry.

METHODS

Healthy third molars with immature and mature root development were formalin-fixed, decalcified in 10% ethylenediaminetetraacetic acid, and processed for routine immunohistochemistry with endothelial cell markers anti-CD34 and anti-CD146 and angiogenic markers anti-vascular endothelial growth factor (VEGF) and anti-VEGF receptor-2 (VEGFR2). Staining was visualized with diaminobenzidine and examined using light microscopy. The distribution of markers was analyzed qualitatively and quantitatively in the coronal, middle, and apical regions of the dentine-pulp complex.

RESULTS

There were spatial differences in protein expression for immature and mature teeth. The pulps of immature teeth were more vascular, had a greater number of CD34+ and CD146+ cells, and a significantly higher MVD in the coronal region than those of mature teeth (P=0.03). The apical papilla contained few blood vessels. VEGF/VEGFR2 activity was significantly greater for immature teeth (P=0.001). VEGF was expressed throughout the pulp-dentine complex, but there was significantly more growth factor coronally (immature P=0.04 and mature P=0.02). VEGFR2 was expressed less than VEGF but was seen on the endothelial cells and single cells unrelated to a vessel lumen.

CONCLUSION

The spatial distribution of vascular and angiogenic (VEGF/VEGFR2) markers indicates the potential for altered healing responses in the pulps of immature and mature teeth. Immature teeth have a greater MVD and VEGF/VEGFR2 expression than mature teeth, and the increased expression of these markers in the coronal region of both tooth types is important for pulp healing.

摘要

目的

采用免疫组织化学方法检测未成熟和成熟恒牙中微血管密度(MVD)、内皮细胞的空间分布及血管生成活性。

方法

将牙根发育未成熟和成熟的健康第三磨牙用福尔马林固定,在10%乙二胺四乙酸中脱钙,然后用内皮细胞标志物抗CD34和抗CD146以及血管生成标志物抗血管内皮生长因子(VEGF)和抗VEGF受体-2(VEGFR2)进行常规免疫组织化学处理。用二氨基联苯胺使染色可视化,并通过光学显微镜检查。在牙髓复合体的冠部、中部和根尖区域对标志物的分布进行定性和定量分析。

结果

未成熟牙和成熟牙的蛋白表达存在空间差异。未成熟牙的牙髓血管更丰富,CD34+和CD146+细胞数量更多,冠部区域的MVD明显高于成熟牙(P=0.03)。根尖乳头血管较少。未成熟牙的VEGF/VEGFR2活性明显更高(P=0.001)。VEGF在整个牙髓-牙本质复合体中均有表达,但冠部的生长因子明显更多(未成熟牙P=0.04,成熟牙P=0.02)。VEGFR2的表达低于VEGF,但在内皮细胞和与血管腔无关的单个细胞上可见。

结论

血管和血管生成(VEGF/VEGFR2)标志物的空间分布表明未成熟和成熟牙髓愈合反应改变的可能性。未成熟牙的MVD和VEGF/VEGFR2表达高于成熟牙,两种牙型冠部区域这些标志物表达的增加对牙髓愈合很重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5fe4/7006575/8fa822a6923f/EEJ-3-153-g001.jpg

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