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关于胃肠外注射纳洛酮单独及联合葡萄糖酸钙对绵羊“钻孔”模型系统骨愈合影响的初步研究。

Preliminary study on the effect of parenteral naloxone, alone and in association with calcium gluconate, on bone healing in an ovine "drill hole" model system.

作者信息

Petrizzi Lucio, Mariscoli Massimo, Valbonetti Luca, Varasano Vincenzo, Langhoff Jens D, Von Rechenberg Brigitte

机构信息

Department of Veterinary Clinical Sciences, University of Teramo, Italy.

出版信息

BMC Musculoskelet Disord. 2007 May 22;8:43. doi: 10.1186/1471-2474-8-43.

Abstract

BACKGROUND

Several diseases affect bone healing and physiology. Many drugs that are commonly used in orthopaedics as "analgesics" or anti-inflammatory agents impair bone healing. Stressful conditions are associated with decreased serum osteocalcin concentration. High endorphin levels alter calcium metabolism, blocking the membrane channels by which calcium normally enters cells. The consequent decrease of intracellular calcium impairs the activities of calcium-related enzymes. Naloxone is a pure opioid antagonist. Morphine-induced osteocalcin inhibition was abolished when osteoblasts were incubated with naloxone. Naloxone restored the altered cellular and tissue physiology by removing beta-endorphins from specific receptors. However, this is only possible if the circulating Ca concentration is adequate. The aim of the present study was to evaluate the efficacy of parenteral naloxone administration in inducing fast mineralization and callus remodelling in a group of sheep with a standardised bone lesion.

METHODS

Twenty ewes were randomly assigned to 4 treatment groups. Group A acted as control, group B received a solution of calcium gluconate, group C a solution of naloxone, and group D a solution of calcium gluconate and naloxone. A transverse hole was drilled in the left metacarpus, including both cortices, then parenteral treatment was administered intramuscularly, daily for four weeks. Healing was evaluated by weekly radiographic examination for eight weeks. For quantitative evaluation, the ratio of the radiographic bone density between the drill area and the adjacent cortical bone was calculated. After eight weeks the sheep were slaughtered and a sample of bone was collected for histopathology

RESULTS

Group D showed a higher radiographic ratio than the other groups. Sheep not treated with naloxone showed a persistently lower ratio in the lateral than the medial cortex (P < 0.01). Histopathology of bone samples showed more caverns and fewer osteoblasts in group D than in the other groups (P </= 0.001).

CONCLUSION

A low-dose parenteral regimen of naloxone enhances mineralization and remodelling of the callus in healing cortical defects in sheep, especially if associated with calcium gluconate.

摘要

背景

多种疾病会影响骨愈合和骨生理。许多在骨科常用作“镇痛药”或抗炎药的药物会损害骨愈合。应激状态与血清骨钙素浓度降低有关。内啡肽水平升高会改变钙代谢,阻断钙正常进入细胞的膜通道。细胞内钙的随之减少会损害钙相关酶的活性。纳洛酮是一种纯阿片类拮抗剂。当成骨细胞与纳洛酮一起孵育时,吗啡诱导的骨钙素抑制作用被消除。纳洛酮通过从特定受体上移除β-内啡肽来恢复改变的细胞和组织生理。然而,只有在循环钙浓度充足时才有可能。本研究的目的是评估在一组有标准化骨损伤的绵羊中,胃肠外给予纳洛酮在诱导快速矿化和骨痂重塑方面的疗效。

方法

将20只母羊随机分为4个治疗组。A组作为对照组,B组接受葡萄糖酸钙溶液,C组接受纳洛酮溶液,D组接受葡萄糖酸钙和纳洛酮溶液。在左掌骨钻一个贯穿两侧皮质的横向孔,然后每周一次肌肉注射进行胃肠外治疗,持续四周。通过每周进行八周的X线检查来评估愈合情况。为了进行定量评估,计算钻孔区域与相邻皮质骨之间的X线骨密度比值。八周后宰杀绵羊,采集骨样本进行组织病理学检查。

结果

D组的X线比值高于其他组。未用纳洛酮治疗的绵羊外侧皮质的比值持续低于内侧皮质(P < 0.01)。骨样本的组织病理学检查显示,D组的空洞比其他组更多,成骨细胞比其他组更少(P≤0.001)。

结论

低剂量胃肠外给予纳洛酮可增强绵羊愈合皮质缺损时骨痂的矿化和重塑,尤其是与葡萄糖酸钙联合使用时。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5131/1891106/760974ab852d/1471-2474-8-43-1.jpg

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