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Effects of dexamethasone on tooth eruption in rats: differences in incisor and molar eruption.

机译:地塞米松对大鼠牙齿萌出的影响:门牙和磨牙萌出的差异。

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A requirement for tooth eruption is the resorption of alveolar bone. Because bone resorption is stimulated by dexamethasone both in vivo and in vitro, dexamethasone 21-phosphate, a soluble form of dexamethasone, was injected into rats to determine its effect on tooth eruption. Such dexamethasone injections accelerate the time of intra-osseous eruption in rat incisors but do not accelerate the eruption time of rat molars when injected into rats. The injections of dexamethasone 21-phosphate also accelerate the time of eyelid opening in the postnatal rats, as well as retarding growth, as measured by body weight. These effects of dexamethasone 21-phosphate parallel the effects of epidermal growth factor injections, including the absence of an effect on molar eruption. This suggests that the molecular signals for the initiation of tooth eruption (i.e., onset of bone resorption) differ between rat incisors and molars. Given that rat incisors are teeth of continuous eruption whereas rat molars are teeth of limited eruption, as are human teeth, care must be taken in extrapolating results derived from rat incisors to human dentition. In vitro, dexamethasone has no effect on the gene expression of either osteoprotegerin or epidermal growth factor in dental follicle cells derived from molars. Because osteoprotegerin expression during normal tooth eruption is transitorily inhibited early postnatally in the molar dental follicle to allow osteoclast formation, the absence of inhibition of its expression by dexamethasone could explain why dexamethasone does not accelerate eruption in molars. Copyright 2001 Wiley-Liss, Inc.
机译:牙齿萌出的要求是牙槽骨的吸收。由于地塞米松在体内和体外均能刺激骨吸收,因此将可溶形式的地塞米松21-磷酸地塞米松21-磷酸酯注入大鼠体内,以确定其对牙齿萌出的作用。这样的地塞米松注射液可加速大鼠切牙的骨内萌发时间,但当其注入大鼠时不会加速大鼠磨牙的萌发时间。注射地塞米松21-磷酸酯还可以加快出生后大鼠眼睑张开的时间,并延缓以体重衡量的生长。地塞米松21-磷酸酯的这些作用与表皮生长因子注射的作用相似,包括对磨牙萌发没有作用。这表明在大鼠切牙和臼齿之间引发牙齿萌发(即骨吸收开始)的分子信号是不同的。鉴于大鼠切牙是连续喷发的牙齿,而大鼠磨牙是有限喷发的牙齿,就像人类的牙齿一样,因此必须谨慎地将源自大鼠切齿的结果外推至人类牙列。在体外,地塞米松对源自臼齿的牙囊细胞中骨保护素或表皮生长因子的基因表达没有影响。由于正常牙齿萌出过程中骨保护素的表达在出生后早期在臼齿牙囊中被暂时抑制,从而导致破骨细胞形成,因此地塞米松对其表达的抑制作用不存在可以解释为什么地塞米松不能促进臼齿的萌发。版权所有2001 Wiley-Liss,Inc.

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