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阿巴洛肽,一种新型的促合成代谢甲状旁腺激素相关肽类似物,通过增加骨形成而不增加骨吸收来增加去势大鼠的皮质骨和小梁骨的骨量和结构。

Abaloparatide, a novel osteoanabolic PTHrP analog, increases cortical and trabecular bone mass and architecture in orchiectomized rats by increasing bone formation without increasing bone resorption.

机构信息

Radius Health, Waltham, MA, USA.

Radius Health, Waltham, MA, USA.

出版信息

Bone. 2019 Mar;120:148-155. doi: 10.1016/j.bone.2018.10.012. Epub 2018 Oct 19.

DOI:10.1016/j.bone.2018.10.012
PMID:30343166
Abstract

Male osteoporosis can occur with advanced age and with hypogonadism, with increased bone resorption and/or inadequate bone formation contributing to reduced bone mass and increased fracture risk. Abaloparatide is a selective PTH receptor agonist that increases bone formation and bone mass in postmenopausal women with osteoporosis and in estrogen-deficient animals. The current study evaluated the effects of abaloparatide in orchiectomized (ORX) rats, a model of male osteoporosis. Four-month-old Sprague-Dawley rats underwent ORX or sham surgery; 8 weeks later the ORX groups exhibited relative osteopenia vs sham controls, based on dual X-ray absorptiometry (DXA) and/or peripheral quantitative computed tomography (pQCT) assessments at the total body, lumbar spine, femur, and tibia. ORX rats (n = 10/group) were then injected daily (s.c.) for 8 weeks with vehicle or abaloparatide at 5 (ABL5) or 25 μg/kg/d (ABL25). Sham controls (n = 10) received s.c. vehicle. DXA and pQCT showed that one or both abaloparatide groups gained more areal and volumetric BMD at all sites analyzed compared with vehicle controls, leading to substantial or complete reversal of ORX-induced BMD deficits. pQCT also indicated greater gains in tibial cortical thickness in both abaloparatide groups versus vehicle controls. Tibial bone histomorphometry showed greater trabecular bone formation and bone volume and improved micro-architecture with abaloparatide, with no increase in osteoclasts. Abaloparatide also led to significant improvements in the balance of biochemical bone formation markers versus bone resorption markers, which correlated with BMD changes. These findings suggest that abaloparatide may have therapeutic benefits in men with osteoporosis.

摘要

男性骨质疏松症可发生于高龄和性腺功能减退症时,其骨吸收增加和/或骨形成不足导致骨量减少和骨折风险增加。阿巴洛肽是一种选择性甲状旁腺激素受体激动剂,可增加骨质疏松症绝经后妇女和去雌激素动物的骨形成和骨量。本研究评估了阿巴洛肽在去势(ORX)大鼠(男性骨质疏松症模型)中的作用。4 月龄 Sprague-Dawley 大鼠接受 ORX 或假手术;8 周后,ORX 组与假对照相比表现出相对骨质疏松症,基于全身、腰椎、股骨和胫骨的双能 X 线吸收法(DXA)和/或外周定量计算机断层扫描(pQCT)评估。然后,将 ORX 大鼠(n=10/组)每天(sc)注射 5(ABL5)或 25μg/kg/d(ABL25)的阿巴洛肽或载体 8 周。假对照(n=10)接受 sc 载体。DXA 和 pQCT 显示,与载体对照组相比,一个或两个阿巴洛肽组在所有分析部位的面积和体积 BMD 均有更多增加,导致 ORX 引起的 BMD 缺陷得到实质性或完全逆转。pQCT 还表明,与载体对照组相比,两个阿巴洛肽组的胫骨皮质厚度均有更大增加。胫骨骨组织形态计量学显示,阿巴洛肽组的小梁骨形成和骨体积增加更多,微结构得到改善,破骨细胞无增加。阿巴洛肽还导致生化骨形成标志物与骨吸收标志物之间的平衡显著改善,这与 BMD 变化相关。这些发现表明,阿巴洛肽可能对男性骨质疏松症患者有治疗益处。

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