用一种新的自动高效液相色谱法评价和比较两种骨丢失大鼠模型-卵巢切除和佐剂性多关节炎-尿吡啶交联

C. Tordjman , A. Lhumeau , P. Pastoureau , F. Meunier , B. Serkiz , J.P. Volland , J. Bonnet
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引用次数: 17

摘要

建立了一种特异性高效液相色谱系统来评估大鼠骨质减少、卵巢切除和佐剂性多关节炎两种模型中胶原交联(吡啶啉(Pyr)和脱氧吡啶啉(D.Pyr))的尿排泄。该方法灵敏度在皮摩尔范围内。去卵巢大鼠骨吸收模型中,Pyr和D.Pyr水平升高较早,在术后2周达到峰值。在整个观察期内(6周),两种水平均保持升高,Pyr/D无变化。Pyr比率。因此,在这个高骨转换模型中,两种交联的平行增加反映了高吸收,导致6周时骨矿物质密度(BMD)显著下降(与对照组相比- 7.3%)。在多发性关节炎大鼠中,在佐剂后2周,Pyr水平与炎症参数平行增加,而D.Pyr水平保持不变。这与我们之前的报道一致,即在辅助治疗后第2周结束时,骨吸收没有变化。从第3周开始,Pyr和D.Pyr均升高。Pyr / D。多发关节炎大鼠Pyr比值均显著增高。这些结果表明,Pyr水平的早期升高反映了非骨性胶原蛋白的分解,当D.Pyr升高时,骨吸收在后期发生,导致骨密度在4周时急剧下降(与对照组相比- 17.7%)。综上所述,我们的研究结果表明,在大鼠和人类中,尿Pyr是骨骼和软骨破坏的标志,而D.Pyr是骨质流失的特定标志。所描述的自动化方法可能构成一个非常有用的工具来评估大鼠骨和/或软骨破坏和评估保护性治疗。
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Evaluation and comparison of urinary pyridinium crosslinks in two rat models of bone loss — ovariectomy and adjuvant polyarthritis — using a new automated HPLC method

A specific HPLC system was developed to assess urinary excretion of collagen crosslinks (pyridinoline (Pyr) and deoxypyridinoline (D.Pyr)) in two models of osteopenia in rats, ovariectomy and adjuvant polyarthritis. The sensitivity of this method was in the picomolar range. In ovariectomized rats, a specific model of bone resorption, Pyr and D.Pyr levels rose early, reaching a peak 2 weeks after surgery. Both levels remained raised during the whole observation period (6 weeks) with no change in the Pyr/D.Pyr ratio. So, in this high bone turnover model, hyperresorption is reflected by the parallel increase of both crosslinks resulting in a significant decrease of bone mineral density (BMD) at 6 weeks (−7.3% vs. control). In polyar-thritic rats, in the 2 post-adjuvant weeks, Pyr levels increased in parallel with inflammatory parameters, whereas D.Pyr levels remained unchanged. This is in agreement with our previous report that at the end of the 2nd week after adjuvant there is no change in bone resorption. From the 3rd week, both Pyr and D.Pyr increased. The Pyr/D.Pyr ratio was always significantly higher in polyarthritic rats. These results suggest that the early increase of Pyr level reflects non-osseous collagen breakdown and that bone resorption occurs at a later stage when D.Pyr rises, leading to a dramatic decrease of BMD at 4 weeks (−17.7% vs. control). Taken together, our results suggest that in rat as in human, urinary Pyr is a marker of bone and cartilage breakdown, whereas D.Pyr is a specific marker of bone loss. This automated method described may constitute a very useful tool to evaluate bone and/or cartilage breakdown in rats and for the assessment of protective treatments.

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Selected bibliography. Socio-economic status and fertility decline: Insights from historical transitions in Europe and North America. Subject index Author index Author index
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