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Acute and long-term effects of corticosteroid therapy on bone metabolism in patients with kidney diseases

机译:皮质类固醇激素治疗对肾脏疾病患者骨代谢的急性和长期影响

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Aim: The aim of our study was to examine parameters of bone metabolism during pulse and long-term methylprednisolone (MP) treatment in patients with kidney diseases. Methods: In 13 patients with RPGN, treated with intravenous MP pulses, followed by tapering oral doses, osteocalcin (OC) and β-CrossLaps (β-CL) were measured before treatment, after the 3rd pulse, then 1 and 3 months later (" acute study" ). In a separate set of analyses serum markers of bone metabolism and bone mineral density (BMD) were studied in 40 patients on maintenance MP therapy (" chronic study" ). Results: Immediately after the 3rd MP pulse serum OC decreased to 38 ± 23%, β-CL increased to 200 ± 121% of the baseline (p = 0.002 for OC and p = 0.003 for β-CL, respectively), and the OC/β-CL ratio decreased from 55 ± 35 to 9 ± 7 (p = 0.002). OC remained below and β-CL above baseline even at 3 months post pulse steroid treatment. Patients in the "chronic study" who were on maintenance oral steroid therapy received 13,844 ± 7,454 mg MP over 53 ± 47 months. BMD at the end of follow-up revealed reduced bone mineral density in 72.5% of the participants. Zscores both at the hip and at the lumbar spine were significantly correlated with duration of steroid treatment and also with the cumulative steroid dose. Conclusion: MP pulse causes immediate, profound suppression of osteoblast function, and significant increase of osteoclast activity, suggesting uncoupling of bone formation and resorption. Prolonged high dose steroid treatment causes significant bone loss in patients with chronic kidney disease. Appropriate systematic follow up of bone metabolism, preventive measures and therapy when needed would be important for the bone health of this patient population.
机译:目的:我们的研究目的是检查肾脏疾病患者的脉冲和长期甲基强的松龙(MP)治疗期间的骨代谢参数。方法:对13例RPGN患者进行静脉MP脉冲治疗,然后逐渐减少口服剂量,在治疗前,第3脉冲后,然后1和3个月后分别测量骨钙素(OC)和β-CrossLaps(β-CL)( “急性研究”)。在另一组分析中,对40名接受维持性MP治疗的患者进行了骨代谢和骨矿物质密度(BMD)血清标志物的研究(“慢性研究”)。结果:在第三个MP脉冲血清OC下降至基线的38±23%之后,β-CL立即上升至基线的200±121%(OC分别为p = 0.002和β-CL分别为p = 0.003)和OC /β-CL比从55±35降低至9±7(p = 0.002)。即使在脉冲类固醇治疗后3个月,OC仍低于基线,β-CL高于基线。在“慢性研究”中接受口服类固醇治疗的患者在53±47个月内接受了13,844±7,454 mg MP。随访结束时的BMD显示72.5%的参与者骨矿物质密度降低。髋部和腰椎的Zscores与类固醇治疗的持续时间以及类固醇累积剂量显着相关。结论:MP脉冲可立即,深刻地抑制成骨细胞的功能,并显着增加破骨细胞的活性,表明骨形成与吸收的解耦。长期服用大剂量类固醇激素会导致慢性肾脏疾病患者的骨质流失。对骨骼代谢进行适当的系统跟进,必要时采取预防措施和治疗对于该患者人群的骨骼健康至关重要。

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