牙周炎
纤维连接蛋白
细胞外基质
牙周组织
医学
糖基化
髓过氧化物酶
血管内皮生长因子
骨膜炎
愤怒(情绪)
内科学
炎症
内分泌学
化学
受体
牙科
生物
血管内皮生长因子受体
生物化学
神经科学
作者
Po‐Chun Chang,Li Yen Chong,Sheng‐Chueh Tsai,Lipyeow Lim
标识
DOI:10.1902/jop.2013.130238
摘要
Background: Advanced glycation end products (AGE) have been found in inflamed gingival tissue and have been shown to interfere with the integrity of extracellular matrix and cell–matrix interactions. This study aims to investigate the modulatory effect of aminoguanidine (AG), an AGE inhibitor, in various stages of experimental periodontitis. Methods: Thirty‐six Sprague‐Dawley rats were used. AG or normal saline (NS) was systemically administered in the induction, progression, and recovery phases of ligature‐induced periodontitis. Dynamic changes of the periodontium were evaluated by microcomputed tomography, histology, and immunohistochemistry of the receptor for AGE (RAGE). Molecular mechanisms were evaluated by myeloperoxidase activity, gene expression of RAGE, and markers associated with tissue repair and homeostasis, including vascular endothelial growth factor (VEGF), type I collagen, fibronectin, and periostin. Results: AG appeared to inhibit the degradation of the collagen matrix in the induction phase but promoted collagen reorganization in the progression and recovery phases of experimental periodontitis. In the induction sites, periodontal bone loss was significantly reduced ( P <0.05), with significantly reduced RAGE ( P <0.05) and significantly elevated fibronectin and periostin levels ( P <0.01). No significant alterations in the levels of myeloperoxidase, VEGF, and collagen were noted. In the progression and recovery sites, similar trends were observed, with insignificant differences relative to NS‐treated animals. Conclusions: AG reduced periodontal bone loss during the induction of experimental periodontitis, and the effects appeared to be insignificant in the progression and recovery phases. This modulation was related to the inhibition of the AGE–RAGE axis to resume cell–matrix interactions and maintain tissue integrity.
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