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阿法骨化醇可恢复去卵巢大鼠的松质骨。

Alfacalcidol restores cancellous bone in ovariectomized rats.

作者信息

Li M, Healy D R, Simmons H A, Ke H Z, Thompson D D

机构信息

Osteoporosis Research, Department of Cardiovascular and Metabolic Diseases, Pfizer Global Research and Development, Groton, CT 06340, USA.

出版信息

J Musculoskelet Neuronal Interact. 2003 Mar;3(1):39-46.

Abstract

Active vitamin D metabolites have been demonstrated to reduce vertebral and hip fractures in elderly patients. A number of in vitro and in vivo pre-clinical studies have suggested that vitamin D may effectively stimulate osteoblastic activity and exert an anabolic effect on bone. The current study was designed to further explore the ability of an active vitamin D analog to restore bone in a skeletal site with established osteopenia in ovariectomized (OVX) rats. Female Sprague Dawley rats at five months of age and 8 weeks after sham ovariectomy or ovariectomy were randomly divided into 7 groups with 10 per group. At the beginning of the treatments, one group of sham-operated rats and one group of OVX rats were sacrificed to serve as baseline controls. Another group of sham-operated rats and one group of OVX rats were treated with vehicle for 4 weeks. The OVX rats in the remaining groups were treated with alfacalcidol at 0.05, 0.1 or 0.2 microg/kg/d by daily oral gavage, 5 days/week for 4 weeks. As expected, estrogen depletion caused high bone turnover and cancellous bone loss in lumbar vertebra of OVX rats. Alfacalcidol treatment at 0.1 or 0.2 but not 0.05 microg/kg/d increased serum calcium and phosphorus in OVX rats as compared with vehicle treatment. In addition, serum parathyroid hormone was suppressed, whereas serum osteocalcin was increased by alfacalcidol at all dose levels. Furthermore, histomorphometric data of 2nd lumbar vertebral body revealed that cancellous bone volume in OVX rats treated with alfacalcidol at 0.1 or 0.2 microg/kg/d was increased to the level of sham-operated rats treated with vehicle. This increment in cancellous bone mass was accompanied by increases in trabecular number and thickness and a decrease in trabecular separation. Moreover, osteoclast surface and number were significantly decreased, whereas bone formation variables such as mineralizing surface and bone formation rate were significantly increased in alfacalcidol- treated OVX rats compared with those of vehicle-treated OVX rats. Finally, a linear regression analysis showed that alfacalcidol treatment dose-dependently altered most of the variables measured in the current study. In conclusion, alfacalcidol completely restores cancellous bone by stimulating bone formation and suppressing bone resorption in lumbar vertebra of OVX rats when the treatment is started at an early phase of osteopenia. The evidence of increased bone formation by alfacalcidol treatments further supports the notion that active vitamin D metabolites or their analogs may exert anabolic effects on bone.

摘要

活性维生素D代谢物已被证明可减少老年患者的椎骨和髋部骨折。多项体外和体内临床前研究表明,维生素D可能有效刺激成骨细胞活性并对骨骼产生合成代谢作用。本研究旨在进一步探讨一种活性维生素D类似物在去卵巢(OVX)大鼠已出现骨质减少的骨骼部位恢复骨量的能力。5月龄、假手术或去卵巢术后8周的雌性Sprague Dawley大鼠被随机分为7组,每组10只。在治疗开始时,处死一组假手术大鼠和一组OVX大鼠作为基线对照。另一组假手术大鼠和一组OVX大鼠用赋形剂治疗4周。其余组的OVX大鼠通过每日口服灌胃给予阿法骨化醇,剂量为0.05、0.1或0.2μg/kg/d,每周5天,共4周。正如预期的那样,雌激素缺乏导致OVX大鼠腰椎骨转换率升高和松质骨丢失。与赋形剂治疗相比,阿法骨化醇以0.1或0.2μg/kg/d而非0.05μg/kg/d的剂量治疗可增加OVX大鼠的血清钙和磷。此外,血清甲状旁腺激素受到抑制,而在所有剂量水平下阿法骨化醇均可使血清骨钙素升高。此外,第二腰椎椎体的组织形态计量学数据显示,用0.1或0.2μg/kg/d阿法骨化醇治疗的OVX大鼠的松质骨体积增加到了用赋形剂治疗的假手术大鼠的水平。松质骨量的增加伴随着小梁数量和厚度的增加以及小梁间距的减小。此外,与赋形剂治疗的OVX大鼠相比,阿法骨化醇治疗的OVX大鼠破骨细胞表面和数量显著减少,而矿化表面和骨形成率等骨形成变量显著增加。最后,线性回归分析表明,阿法骨化醇治疗剂量依赖性地改变了本研究中测量的大多数变量。总之,当在骨质减少的早期阶段开始治疗时,阿法骨化醇通过刺激骨形成和抑制OVX大鼠腰椎的骨吸收来完全恢复松质骨。阿法骨化醇治疗增加骨形成的证据进一步支持了活性维生素D代谢物或其类似物可能对骨骼产生合成代谢作用的观点。

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