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Equilibrium-dependent bisphosphonate interaction with crystalline bone mineral explains anti-resorptive pharmacokinetics and prevalence of osteonecrosis of the jaw in rats

机译:平衡依赖性双膦酸酯与结晶性骨矿物质的相互作用解释了大鼠下颌骨的骨吸收和抗吸收药代动力学

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Bisphosphonates (BPs) are chemically stable analogs of pyrophosphate exhibiting strong affinity to bone and have been used for the treatment of diseases characterized by excessive bone resorption. Contrary to the widely accepted BP accumulation model in bone after repeated applications, we report here that an equilibrium-dependent BP-crystalline bone mineral interaction may better explain BP bio-distribution and anti-catabolic bone remodeling and may be relevant to the appearance of osteonecrosis of the jaw (ONJ) in rats. Fluorescent-labeled BP analogs were synthesized and used to evaluate the mode of bone adsorption. After fluorescent-labeled BP adsorbed on crystalline calcium phosphates in vitro, subsequent BP application replaced the previously absorbed BP depending on the dose and the relative binding affinity to hydroxyapatite. The in vivo intravenous zoledronate (ZOL) injection of repeated fractional doses resulted in lower serum CTX and TRAP5b measurements than a single bolus injection in spite of the equivalent cumulative dose. Repeated injections resulted in the distribution of fluorescent-labeled BP on the large area of bone surfaces; whereas the single bolus injection gave rise to the intense BP bio-distribution at selected bone sites such as the alveolar process of jawbones. Necrotic maxillary alveolar bone was predominantly observed in vitamin D deficiency rats treated with bolus ZOL injection. The palatal necrotic bone was characteristically sequestrated by the fistulation of hyperplastic oral epithelium, suggesting the initial development of ONJ-like lesions in rats. Our results suggest that equilibrium-dependent BP-bone interaction may, in part, determine the effectiveness and influence side effects of long-term and repeated applications of BPs. ? 2012 Elsevier Inc.
机译:双膦酸盐(BPs)是焦磷酸酯的化学稳定的类似物,对骨骼具有很强的亲和力,已被用于治疗以骨骼过度吸收为特征的疾病。与重复应用后在骨骼中广泛接受的BP堆积模型相反,我们在这里报告,依赖于平衡的BP晶体与骨矿物质的相互作用可能更好地解释了BP的生物分布和抗分解代谢的骨骼重塑,并且可能与骨坏死的出现有关大鼠的颌骨(ONJ)。合成了荧光标记的BP类似物,并用于评估骨吸收的模式。荧光标记的BP在体外吸附到结晶磷酸钙上后,随后的BP应用取决于剂量和对羟基磷灰石的相对结合亲和力,取代了先前吸收的BP。尽管累积剂量相等,但重复小剂量的体内静脉注射唑来膦酸盐(ZOL)注射仍比单次大剂量注射产生的血清CTX和TRAP5b降低。重复注射导致荧光标记的BP在大面积骨表面上分布。而单次推注则在选定的骨骼部位(如颚骨的牙槽突)引起了强烈的BP生物分布。在推注ZOL注射治疗的维生素D缺乏症大鼠中,主要观察到坏死的上颌牙槽骨。增生的口腔上皮的瘘管将characteristic骨坏死骨隔离,提示大鼠出现了ONJ样病变。我们的结果表明,依赖于平衡的BP骨相互作用可能部分决定长期和重复使用BP的有效性并影响其副作用。 ? 2012爱思唯尔公司

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