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抗硬骨素抗体和机械加载似乎独立影响大鼠干骺端骨。

Anti-sclerostin antibody and mechanical loading appear to influence metaphyseal bone independently in rats.

机构信息

Orthopaedics Division, Department of Clinical and Experimental Medicine, Faculty of Medicine, Linköping University, Sweden.

出版信息

Acta Orthop. 2011 Oct;82(5):628-32. doi: 10.3109/17453674.2011.625539.

Abstract

BACKGROUND AND PURPOSE

Sclerostin is produced by osteocytes and is an inhibitor of bone formation. Thus, inhibition of sclerostin by a monoclonal antibody increases bone formation and improves fracture repair. Sclerostin expression is upregulated in unloaded bone and is downregulated by loading. We wanted to determine whether an anti-sclerostin antibody would stimulate metaphyseal healing in unloaded bone in a rat model.

METHODS

10-week-old male rats (n = 48) were divided into 4 groups, with 12 in each. In 24 rats, the right hind limb was unloaded by paralyzing the calf and thigh muscles with an injection of botulinum toxin A (Botox). 3 days later, all the animals had a steel screw inserted into the right proximal tibia. Starting 3 days after screw insertion, either anti-sclerostin antibody (Scl-Ab) or saline was given twice weekly. The other 24 rats did not receive Botox injections and they were treated with Scl-Ab or saline to serve as normal-loaded controls. Screw pull-out force was measured 4 weeks after insertion, as an indicator of the regenerative response of bone to trauma.

RESULTS

Unloading reduced the pull-out force. Scl-Ab treatment increased the pull-out force, with or without unloading. The response to the antibody was similar in both groups, and no statistically significant relationship was found between unloading and antibody treatment. The cancellous bone at a distance from the screw showed changes in bone volume fraction that followed the same pattern as the pull-out force.

INTERPRETATION

Scl-Ab increases bone formation and screw fixation to a similar degree in loaded and unloaded bone.

摘要

背景与目的

骨硬化蛋白由骨细胞产生,是骨形成的抑制剂。因此,单克隆抗体抑制骨硬化蛋白可增加骨形成并改善骨折修复。骨硬化蛋白在未负重的骨中表达上调,并可被负重所下调。我们希望确定抗骨硬化蛋白抗体是否会在大鼠模型中刺激未负重骨的骺端愈合。

方法

将 10 周龄雄性大鼠(n = 48)分为 4 组,每组 12 只。在 24 只大鼠中,通过注射肉毒杆菌毒素 A(Botox)麻痹小腿和大腿肌肉使右侧后肢失用。3 天后,所有动物的右侧胫骨近端均插入一根钢钉。自插入钢钉后 3 天开始,每周两次给予抗骨硬化蛋白抗体(Scl-Ab)或生理盐水。另外 24 只大鼠未接受 Botox 注射,并用 Scl-Ab 或生理盐水处理作为正常负重对照。插入 4 周后测量螺钉拔出力,作为骨对创伤再生反应的指标。

结果

失用减少了拔出力。Scl-Ab 治疗增加了拔出力,无论是否失用。两组对抗体的反应相似,并且在失用和抗体治疗之间未发现统计学上显著的关系。远离螺钉的松质骨的骨体积分数变化遵循与拔出力相同的模式。

结论

Scl-Ab 在负重和未负重的骨中以相似的程度增加骨形成和螺钉固定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f8e7/3242963/6daf70326e3a/ORT-0300-9734-082-628_g001.jpg

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