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Frequent administration of abaloparatide shows greater gains in bone anabolic window and bone mineral density in mice: A comparison with teriparatide

机译:常常捕气的鲍鱼肽在骨骼合成代谢窗口和小鼠中的骨矿物密度方面显示出更大的成果:与萜壶肽的比较

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摘要

Abaloparatide (ABL) is a novel 34-amino acid peptide analog of parathyroid hormone-related protein. In clinical studies, although ABL showed a greater bone mineral density (BMD) increase than teriparatide (TPTD, human parathyroid hormone 1-34), the responses of ABL to bone formation and resorption markers were weaker, making it difficult to understand the relationship between the bone anabolic window (increase in bone formation versus resorption) and bone mass. In the present study, the effects of ABL and TPTD were compared in mice. Given that the rate of bone turnover is higher in rodents than in humans, the comparison was made with several administration regimens providing equivalent daily dosages: once daily (QD, 30 mu g/kg every 24 h), twice daily (BID, 15 mu g/kg every 12 h), or three times a day (TID, 10 mu g/kg every 8 h). Frequent administration of ABL showed higher BMD with enhancement of trabecular and cortical bone mass and structures than that of TPTD, consistent with the clinical results seen with once daily administration. ABL increased bone formation marker levels more than TPTD with more frequent regimens, while bone resorption marker levels were not different between ABL and TPTD in all regimens. Analysis of bone histomorphometry and gene expression also suggested that ABL increased bone formation more than TPTD, while the effect on bone resorption was almost comparable between ABL and TPTD. The bone anabolic windows calculated from bone turnover markers indicated that ABL enhanced the anabolic windows more than TPTD, leading to a robust increase in BMD. The mechanism by which ABL showed a better balance of bone turnover was suggested to be partly due to the enhanced remodeling-based bone formation involved in Ephb4. Taken together, our findings would help elucidate the mechanism by which ABL shows excellent BMD gain and reduction of fractures in patients with osteoporosis.
机译:鲍鱼(ABL)是甲状旁腺激素相关蛋白的新型34-氨基酸肽类似物。在临床研究中,虽然ABL显示比Teriparatide更大的骨矿物密度(BMD)增加(TPTD,人甲状旁腺激素1-34),但ABL与骨形成和吸收标记的反应较弱,使得难以理解之间的关系骨骼合成代谢窗口(骨形成增加而吸收)和骨质量。在本研究中,在小鼠中比较ABL和TPTD的效果。鉴于啮齿动物的骨质营业额较高比人类更高,对多种管理方案进行了比较,提供了当量的日常剂量:每日一次(每24小时QD,30μg/ kg),每日两次(出价,15亩g / kg每12小时,或每天三次(每8小时10μg/ kg)。常常施用ABL显示出高比例和皮质骨质量和结构的较高BMD,而不是TPTD,与每日一次施用一次的临床结果一致。 ABL增加骨形成标记水平超过TPTD,具有更频繁的方案,而骨吸收标记水平在所有方案中的ABL和TPTD之间没有差异。骨组织形态和基因表达的分析还表明ABL增加了骨形成超过TPTD,而对骨吸收的影响几乎相当于ABL和TPTD。由骨移植标记计算的骨骼合成代谢窗表明ABL增强了多于TPTD的合成窗口,导致BMD的强大增加。 Abl显示出更好的骨转换平衡的机制是部分原因是由于ephb4中涉及增强的基于重塑的骨形成。我们的研究结果将有助于阐明ABL在骨质疏松症患者中表现出优异的BMD增益和减少骨折的机制。

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