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甲状旁腺激素和生长激素在用于已患骨质减少的去卵巢大鼠的干预治疗时具有相加或协同作用。

Parathyroid hormone and growth hormone have additive or synergetic effect when used as intervention treatment in ovariectomized rats with established osteopenia.

作者信息

Mosekilde L, Tornvig L, Thomsen J S, Orhii P B, Banu M J, Kalu D N

机构信息

Department of Cell Biology, Institute of Anatomy, University of Aarhus, Arhus, Denmark.

出版信息

Bone. 2000 Jun;26(6):643-51. doi: 10.1016/s8756-3282(00)00276-3.

Abstract

The severely osteoporotic human skeleton is characterized by thin cortices and a very fragile cancellous framework. To increase the biomechanical competence of such a skeleton, powerful anabolic agents are needed. The aim of the present study was to compare the effect of parathyroid hormone (PTH), growth hormone (GH) and combination treatment with PTH and GH in an aged, rat model with established osteopenia. Furthermore, envelope- and site-specific effects of the two agents are described. Twelve-month-old virgin F344 rats were divided into six groups with 11 animals per group: (1) baseline; (2) sham-operated + solvent vehicle (s.v.) (sham); (3) ovariectomized + s.v. (ovx); (4) ovx + GH 2.5 mg/kg body weight per day; (5) ovx + PTH 80 microg/kg body weight per day; and (6) ovx + GH and PTH treatment. Group 1 were killed to establish baseline values. Groups 2 (sham) and 3 (ovx) were killed after 24 weeks. Groups 4, 5, and 6 were allowed to develop osteopenia for 16 weeks before treatment was initiated. Treatment was given for a period of 8 weeks. The effects of GH, PTH, and GH + PTH cotherapy were measured by biomechanical testing at four different skeletal sites: lumbar vertebra; femoral diaphysis; femoral neck; and distal femoral metaphysis. In addition, static histomorphometry was performed at the middiaphyseal region. Ovx induced a loss of bone strength at all sites, but this was significant only at the femoral diaphysis and distal metaphysis. GH could reverse the loss of strength at the diaphysis, but not at the metaphysis. PTH, on the other hand, reversed the loss of strength to values significantly over ovx at all four sites. At the metaphysis, PTH monotherapy increased strength to above sham levels. However, GH + PTH cotherapy showed additive or synergistic effects at the four tested sites, leading to strength values significantly over sham at all these sites. Static histomorphometry showed that GH exerted its main effect on the periosteal envelope and PTH on the endocortical envelope; for this reason, the GH + PTH combination treatment had an additive or synergistic effect. We conclude that GH and PTH have a very pronounced anabolic effect when given in cotherapy. Therefore, this treatment regime seems promising in the clinical situation for management of patients with severe, established osteoporosis.

摘要

严重骨质疏松的人体骨骼具有皮质薄和松质骨框架非常脆弱的特点。为了提高这种骨骼的生物力学性能,需要强效的合成代谢药物。本研究的目的是比较甲状旁腺激素(PTH)、生长激素(GH)以及PTH与GH联合治疗对已建立骨质减少的老年大鼠模型的影响。此外,还描述了这两种药物的包膜特异性和部位特异性作用。将12月龄的未交配F344大鼠分为6组,每组11只动物:(1)基线组;(2)假手术+溶剂载体(s.v.)(假手术组);(3)卵巢切除+ s.v.(去卵巢组);(4)去卵巢+每天2.5 mg/kg体重的GH;(5)去卵巢+每天80 μg/kg体重的PTH;(6)去卵巢+GH和PTH联合治疗组。第1组处死以确定基线值。第2组(假手术组)和第3组(去卵巢组)在24周后处死。第4、5和6组在开始治疗前让骨质减少发展16周。治疗持续8周。通过在四个不同骨骼部位进行生物力学测试来测量GH、PTH和GH + PTH联合治疗的效果:腰椎;股骨干;股骨颈;以及股骨远端干骺端。此外,在骨干中部区域进行静态组织形态计量学分析。去卵巢导致所有部位的骨强度下降,但仅在股骨干和远端干骺端有显著下降。GH可逆转骨干处的强度下降,但不能逆转干骺端处的下降。另一方面,PTH可将所有四个部位的强度下降逆转至显著高于去卵巢组的值。在干骺端,PTH单一疗法可使强度增加到高于假手术组的水平。然而,GH + PTH联合治疗在四个测试部位显示出相加或协同作用,导致所有这些部位的强度值显著高于假手术组。静态组织形态计量学表明,GH主要作用于骨膜包膜,PTH主要作用于内皮质包膜;因此,GH + PTH联合治疗具有相加或协同作用。我们得出结论,GH和PTH联合治疗时具有非常显著的合成代谢作用。因此,这种治疗方案在临床治疗严重的、已确诊的骨质疏松症患者方面似乎很有前景。

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