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卵巢切除大鼠的松质骨量和骨连接性丧失可通过甲状旁腺激素和雌二醇联合治疗得以恢复。

Loss of cancellous bone mass and connectivity in ovariectomized rats can be restored by combined treatment with parathyroid hormone and estradiol.

作者信息

Shen V, Dempster D W, Birchman R, Xu R, Lindsay R

机构信息

Regional Bone Center, Helen Hayes Hospital, New York State Department of Health, W. Haverstraw 10993.

出版信息

J Clin Invest. 1993 Jun;91(6):2479-87. doi: 10.1172/JCI116483.

Abstract

To evaluate the potential use of a combination of antiresorption and bone formation-promoting agents as a treatment for postmenopausal osteoporosis, we examined the effects of combined and separate administration of estrogen (17 beta-estradiol, 30 micrograms/kg per d, s.c.) and parathyroid hormone (rPTH [1-34], 40 micrograms/kg per d, s.c.) on the proximal tibia of ovariectomized (Ovx) rats. The treatments lasted for 4 wk and were initiated 1, 3, and 5 wk after surgery. Ovx resulted in rapid loss of cancellous bone volume (Cn-BV/TV) as well as trabecular connectivity, as determined by two dimensional strut analysis. When administered in a preventive mode, treatment beginning 1 wk post-Ovx, estrogen or PTH treatment alone preserved Cn-BV/TV and trabecular connectivity, and combined estrogen and PTH treatment caused a 40% increment in Cn-BV/TV while maintaining comparable trabecular connectivity with that seen in the Sham-operated animals. When administered in a curative mode to rats with established osteoporosis, treatments beginning 3 or 5 wk post-Ovx, estrogen or PTH treatment alone prevented further loss of connectivity and Cn-BV/TV, whereas the combined treatment resulted in as much as a 300% improvement in one of the parameters of trabecular connectivity, node to node strut length, and a 106% increase in Cn-BV/TV, with respect to the bone status at the initiation of treatment. The beneficial effects of this combined treatment derive from estrogen's ability to prevent accelerated bone resorption and, simultaneously, PTH's promotion of bone formation. These data demonstrate, in an animal model, that therapies can be devised to cure the skeletal defects associated with established osteoporosis.

摘要

为评估抗骨吸收和促骨形成药物联合使用治疗绝经后骨质疏松症的潜在用途,我们研究了雌激素(17β-雌二醇,30微克/千克/天,皮下注射)和甲状旁腺激素(重组人甲状旁腺激素[1-34],40微克/千克/天,皮下注射)联合及单独给药对去卵巢(Ovx)大鼠胫骨近端的影响。治疗持续4周,于手术后1、3和5周开始。通过二维支柱分析确定,Ovx导致松质骨体积(Cn-BV/TV)以及小梁连接性迅速丧失。在预防性给药模式下,Ovx后1周开始治疗,单独使用雌激素或甲状旁腺激素治疗可保留Cn-BV/TV和小梁连接性,雌激素和甲状旁腺激素联合治疗使Cn-BV/TV增加40%,同时保持与假手术动物相当的小梁连接性。在对已患骨质疏松症的大鼠进行治疗性给药时,Ovx后3或5周开始治疗,单独使用雌激素或甲状旁腺激素治疗可防止连接性和Cn-BV/TV进一步丧失,而联合治疗使小梁连接性的一个参数(节点到节点支柱长度)提高多达300%,Cn-BV/TV相对于治疗开始时的骨状态增加106%。这种联合治疗的有益效果源于雌激素预防加速骨吸收的能力,以及同时甲状旁腺激素促进骨形成的能力。这些数据在动物模型中表明,可以设计出治疗方法来治愈与已患骨质疏松症相关的骨骼缺陷。

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