慢性酒精滥用大鼠模型中低剂量甲状旁腺激素对腰椎的影响。
The effects of low dose parathyroid hormone on lumbar vertebrae in a rat model for chronic alcohol abuse.
机构信息
Department of Nutrition and Exercise Sciences, Oregon State University, 107d Milam Hall, Corvallis, OR 97331, USA.
出版信息
Osteoporos Int. 2011 Apr;22(4):1175-81. doi: 10.1007/s00198-010-1304-4. Epub 2010 Jun 12.
UNLABELLED
This study evaluated the hypothesis that increased bone marrow adipogenesis is coupled to decreased bone formation in rats consuming alcohol. Parathyroid hormone (PTH) increased bone formation but had no effect on marrow adiposity. We conclude that increased adiposity does not prevent the bone anabolic response to PTH.
INTRODUCTION
Alcoholism results in decreased bone formation and increased bone marrow adiposity. The present study tested the hypothesis that these reciprocal changes are coupled by evaluating the effect of intermittent PTH on bone formation and bone marrow adiposity in a rat model for chronic alcohol abuse.
METHODS
Three-month-old male Sprague Dawley rats (n = 10-11/group) were fed the Lieber-DeCarli liquid diet with 35% of the calories derived from ethanol. Control rats were pair-fed an isocaloric alcohol-free diet. The rats were administered low dose PTH (1 µg/kg/day sc, 5 d/week) or vehicle for 6 weeks. Cancellous bone architecture in lumbar vertebrae was evaluated by micro-computed tomography followed by histomorphometric assessment of bone formation and marrow adiposity.
RESULTS
Alcohol increased bone marrow adiposity but reduced bone formation. The latter was due to decreases in mineralizing perimeter/bone perimeter, a surrogate measure of osteoblast number, and mineral apposition rate, a measure of osteoblast activity. PTH increased bone formation by increasing mineralizing perimeter/bone perimeter. In contrast, PTH had no effect on mineral apposition rate or bone marrow adiposity. Interactions between alcohol consumption and PTH treatment were not detected for any endpoints evaluated.
CONCLUSIONS
PTH treatment blunted the decrease in mineralizing perimeter/bone perimeter in alcohol-fed rats but was ineffective in preventing the increase in bone marrow adiposity. These findings suggest that the alcohol-induced increase in adipocytes is not directly responsible for the accompanying reduction in bone formation.
目的
本研究旨在验证下述假说,即酒精摄入大鼠的骨髓脂肪生成增加与成骨减少相关。甲状旁腺激素(PTH)可增加骨形成,但对骨髓脂肪含量无影响。我们的结论为,脂肪含量增加不会阻止 PTH 对骨骼的合成代谢作用。
引言
酒精摄入会导致骨形成减少和骨髓脂肪增加。本研究通过评估间歇给予 PTH 对慢性酒精滥用大鼠模型中骨形成和骨髓脂肪含量的影响,对上述假说进行了验证。
方法
3 月龄雄性 Sprague Dawley 大鼠(n = 10-11/组)给予 Lieber-DeCarli 液体饲料,其中 35%的热量来自乙醇。对照组大鼠给予等热量不含酒精的饲料。大鼠接受低剂量 PTH(1 µg/kg/天,sc,每周 5 天)或载体治疗 6 周。腰椎松质骨结构通过微计算机断层扫描评估,随后进行骨形成和骨髓脂肪含量的组织形态计量学评估。
结果
酒精增加了骨髓脂肪含量,但减少了骨形成。后者是由于矿化周长/骨周长减少所致,这是成骨细胞数量的替代指标,以及矿化速率,这是成骨细胞活性的指标。PTH 通过增加矿化周长/骨周长来增加骨形成。相比之下,PTH 对矿化速率或骨髓脂肪含量没有影响。未检测到任何评估终点的酒精摄入与 PTH 治疗之间的相互作用。
结论
PTH 治疗可减轻酒精喂养大鼠矿化周长/骨周长的减少,但不能预防骨髓脂肪含量的增加。这些发现表明,酒精引起的脂肪细胞增加并不是伴随骨形成减少的直接原因。
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