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首页> 外文期刊>Bone >Effects of suppressed bone remodeling by minodronic acid and alendronate on bone mass, microdamage accumulation, collagen crosslinks and bone mechanical properties in the lumbar vertebra of ovariectomized cynomolgus monkeys
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Effects of suppressed bone remodeling by minodronic acid and alendronate on bone mass, microdamage accumulation, collagen crosslinks and bone mechanical properties in the lumbar vertebra of ovariectomized cynomolgus monkeys

机译:小乳酸和醛酮酸酯对卵黄骨质,微岩积累,胶原骨质交联和骨骼机械性能抑制骨质重塑的影响

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摘要

Collagen crosslinking is an important determinant of the quality of bone material. We have previously shown that suppressed bone turnover by high doses of minodronic acid and alendronate increases compressive strength of vertebra, but also increases microdamage accumulation, in monkey bone. The aim of this study is to examine the effects of these bisphosphonates on collagen crosslinks and intrinsic material properties, in addition to microdamage accumulation, in vertebral cancellous bone in ovariectomized cynomolgus monkeys. Sixty female monkeys aged 9-17 years were divided into five groups: sham and ovariectomized groups were treated daily for 17 months with lactose vehicle, and the other three groups were given minodronic acid daily at 0.015 or 0.15 mg/kg or alendronate daily at 0.5 mg/kg orally. After sacrifice, lumbar vertebrae were subjected to histomorphometry, microdamage measurement, analysis of collagen crosslinking and compressive mechanical tests. Minodronic acid caused dose-dependent suppression of increased bone remodeling due to ovariectomy, and low-dose minodronic acid suppressed remodeling same level as alendronate. However, low-dose minodronic acid did not change microdamage accumulation, collagen maturity and the pentosidine level, whereas high-dose minodronic acid and alendronate increased these parameters. Compressive ultimate load was increased following high-dose minodronic acid and alendronate, but no treatment altered the reduction in intrinsic material properties caused by ovariectomy. These findings suggest that deterioration of bone material and formation of pentosidine and microdamage induced by minodronic acid is less than that expected based on the extent of remodeling suppression, in comparison with alendronate, but this was not reflected in any significant change of mechanical properties. (C) 2017 Elsevier Inc. All rights reserved.
机译:胶原蛋白交联是骨材料质量的重要决定因素。我们之前已经表明,通过高剂量的小剂量的小剂量抑制椎体的骨质成交量增加了椎体的抗压强度,而且还增加了猴骨中的微水池积累。本研究的目的是检查这些双膦酸盐对胶原交联和内在材料特性的影响,除了微米切除术中的椎体松散骨中的微量沸石积累。 9-17岁的六十雌性猴子分为五组:假时和卵巢切除群体每天用乳糖载体治疗17个月,另外三组每天在0.015或0.15mg / kg或每日2015或0.15mg / kg或alendronate时给予minodronic an。 mg / kg口服。牺牲后,对腰椎进行腰椎,微水力解测量,分析胶原交联和压缩机械试验。小铁酸导致剂量依赖性抑制由于卵巢切除术管增加的骨重塑,低剂量小剂量酸抑制了与醛膦酸盐相同的水平。然而,低剂量的小透射酸不改变微米沸腾积累,胶原蛋白成熟度和戊糖氨酸水平,而高剂量的小剂量和醛酸酯增加这些参数。高剂量小剂量酸和醛固酸盐后,压缩终极载荷增加,但没有治疗改变了由卵巢切除术引起的内在材料特性的降低。这些发现表明,基于反弹批准的重塑抑制程度,骨材料的损坏和由小碳酸诱导的戊糖苷和微量沸石的形成小于预期,但与醛膦酸盐相比,这不会反映在机械性能的任何显着变化中。 (c)2017年Elsevier Inc.保留所有权利。

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