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长期唑来膦酸治疗可增加去卵巢成年大鼠长骨的骨结构和力学强度。

Long-term zoledronic acid treatment increases bone structure and mechanical strength of long bones of ovariectomized adult rats.

作者信息

Hornby S B, Evans G P, Hornby S L, Pataki A, Glatt M, Green J R

机构信息

Biomedical Research, AEA Technology, 551 Harwell, Didcot, Oxfordshire, OX11 ORA, UK.

出版信息

Calcif Tissue Int. 2003 Apr;72(4):519-27. doi: 10.1007/s00223-002-2015-4. Epub 2003 Feb 10.

Abstract

Zoledronic acid (ZOL) is a highly potent heterocyclic bisphosphonate which has been shown to inhibit bone resorption in short-term experiments in young growing animals. In this investigation we have evaluated the effects of a 1-year administration to mature, ovariectomized (OVX) rats as a model for postmenopausal osteoporosis in order to elucidate (1) the temporal changes in urinary biochemical markers of bone turnover and femoral bone mineral density (BMD), (2) to measure changes of static and dynamic histomorphometric parameters and mechanical strength, and (3) to assess the preventive effects of chronic treatment with ZOL on these parameters. In urine, deoxypyridinoline increased after OVX and was significantly reduced by ZOL administration, indicative of a reduced bone collagen turnover. These changes were accompanied by alterations of tibial cancellous bone: trabecular bone volume and parameters of bone architecture were significantly augmented by ZOL and bone formation rates fell as a consequence of suppressed bone turnover, but were still measurable. No signs of "frozen bone" or osteomalacia could be detected. BMD of the whole femurs rose in sham-operated control animals (SHAM) during the entire experimental period, whereas in OVX animals, BMD plateaued after 32 weeks at a lower level. ZOL at a low dose (0.3 mg/kg/week s.c.) did not alter whole femur BMD, but at higher doses (1.5 and 7.5 mg/kg/week s.c.) BMD increased to the level of the SHAM group. A distinct pattern was noted for the distal quarter of the femur, a region rich in cancellous bone: BMD initially increased in all treatment groups except the OVX group, and at a later stage fell again at a comparable rate irrespective of treatment. Mechanical stability, as assessed by a 3-point bending test, was significantly increased by all doses of ZOL and exceeded OVX and sham-operated controls. The effects on mechanical properties were observed at a low dose which did not measurably increase femoral BMD after 1-year treatment. Multiregression analysis revealed a significant positive correlation between maximum load and BMD, and a significant negative correlation of maximum load with labeled perimeter, a marker of bone formation and turnover. No significant correlation was found with urinary deoxypyridinoline, a marker of bone resorption. The data show that mechanical testing detects improvements of functional bone quality following low dose bisphosphonate treatment which are not identified by standard DXA measurements of BMD.

摘要

唑来膦酸(ZOL)是一种高效的杂环双膦酸盐,在对幼年生长动物的短期实验中已显示出能抑制骨吸收。在本研究中,我们评估了对成熟的去卵巢(OVX)大鼠进行为期1年的给药效果,以此作为绝经后骨质疏松症的模型,以阐明:(1)骨转换的尿生化标志物和股骨骨矿物质密度(BMD)的时间变化;(2)测量静态和动态组织形态计量学参数及力学强度的变化;(3)评估ZOL长期治疗对这些参数的预防作用。在尿液中,去氧吡啶啉在OVX后增加,而通过给予ZOL显著降低,这表明骨胶原转换减少。这些变化伴随着胫骨松质骨的改变:ZOL使小梁骨体积和骨结构参数显著增加,由于骨转换受抑制,骨形成率下降,但仍可测量。未检测到“骨冻结”或骨软化的迹象。在整个实验期间,假手术对照动物(SHAM)的全股骨BMD升高,而在OVX动物中,BMD在32周后达到平台期且处于较低水平。低剂量(0.3 mg/kg/周皮下注射)的ZOL未改变全股骨BMD,但较高剂量(1.5和7.5 mg/kg/周皮下注射)时BMD增加到SHAM组的水平。在富含松质骨的股骨远端四分之一区域观察到一种独特的模式:除OVX组外,所有治疗组的BMD最初均增加,且在后期以相似的速率再次下降,与治疗无关。通过三点弯曲试验评估的力学稳定性,所有剂量的ZOL均使其显著增加,且超过OVX组和假手术对照组。在为期1年的治疗后,低剂量ZOL未使股骨BMD有可测量的增加,但观察到其对力学性能有影响。多元回归分析显示最大负荷与BMD之间存在显著正相关,最大负荷与标记周长(骨形成和转换的标志物)之间存在显著负相关。未发现与骨吸收标志物尿去氧吡啶啉有显著相关性。数据表明,力学测试可检测到低剂量双膦酸盐治疗后功能性骨质量的改善,而标准双能X线吸收法(DXA)测量BMD无法识别这些改善。

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