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Anatomic site variability in rat skeletal uptake and desorption of fluorescently labeled bisphosphonate.

机译:大鼠骨骼摄取和荧光标记的双膦酸盐的解剖学位点变异性。

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OBJECTIVES: Bisphosphonates commonly used to treat osteoporosis, Paget's disease, multiple myeloma, hypercalcemia of malignancy and osteolytic lesions of cancer metastasis have been associated with bisphosphonate-associated jaw osteonecrosis (BJON). The underlying pathogenesis of BJON is unclear, but disproportionate bisphosphonate concentration in the jaw has been proposed as one potential etiological factor. This study tested the hypothesis that skeletal biodistribution of intravenous bisphosphonate is anatomic site-dependent in a rat model system. MATERIALS AND METHODS: Fluorescently labeled pamidronate was injected intravenously in athymic rats of equal weights followed by in vivo whole body fluorimetry, ex vivo optical imaging of oral, axial, and appendicular bones and ethylenediaminetetraacetic acid bone decalcification to assess hydroxyapatite-bound bisphosphonate. RESULTS: Bisphosphonate uptake and bisphosphonate released per unit calcium were similar in oral and appendicular bones but lower than those in axial bones. Hydroxyapatite-bound bisphosphonate liberated by sequential acid decalcification was the highest in oral, relative to axial and appendicular bones (P < 0.05). CONCLUSIONS: This study demonstrates regional differences in uptake and release of bisphosphonate from oral, axial, and appendicular bones of immune deficient rats.
机译:目的:常用于治疗骨质疏松症,Paget疾病,多发性骨髓瘤,恶性肿瘤的高钙血症的双膦酸盐与癌症转移的骨质疏松病变的高钙血症已经与双膦酸盐相关的颌骨骨折(Bjon)有关。 BJON的潜在发病机制不明显,但是,已经提出了钳口中的双膦酸盐浓度作为一种潜在的病因因子。该研究测试了静脉内双膦酸盐的骨骼生物分布的假设是依赖于大鼠模型系统的解剖学位点。材料和方法:荧光标记的氨基磺酸盐在相等重量的无甲醛大鼠中静脉内注射,然后体内全身荧光测量,口服,轴向和阑尾骨的离体光学成像和乙二胺四乙酸骨脱钙,以评估羟基磷灰石 - 结合的双膦酸盐。结果:每单位钙释放的双膦酸盐摄取和双膦酸盐在口腔和附奇骨骼中相似,但低于轴骨骨的骨骼。通过顺序酸性脱钙释放的羟基磷灰石 - 结合的双膦酸盐在口腔中最高,相对于轴向和附奇骨骼(P <0.05)。结论:本研究表明,来自免疫缺陷大鼠的口服,轴向和骨骼的摄取和释放双膦酸盐的区域差异。

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