[周期性口服依地膦酸盐治疗类固醇性骨质疏松症对骨密度的临床益处]。

Ryumachi. [Rheumatism] Pub Date : 2002-08-01
Tomoko Nakamura, Soichiro Maekawa, Sahoko Morinobu, Akio Morinobu, Masahiro Koshiba, Mika Yamauchi, Toshitsugu Sugimoto, Shunichi Kumagai
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引用次数: 0

摘要

目的:比较不同风湿病伴皮质激素所致骨质疏松患者间歇性循环替地膦酸钠对骨量的影响。患者和方法:我们评估了34例长期使用皮质类固醇(> 6个月)的女性患者(平均年龄:46.4±13.7岁,17-71岁)腰椎骨密度(BMD)。18例患者周期性口服地替膦酸盐(每天400 mg或200 mg地替膦酸盐,持续2周,随后10-12周无药期)。在这18例患者中,12例接受400 mg/d (A组)治疗,另外6例接受200 mg/d (B组)治疗。16例未使用地替膦酸盐的患者作为对照组。结果:依地膦酸钠周期性治疗可显著提高骨密度。12个月后,A组患者的腰椎骨密度从0.760 +/- 0.10 g/ cm2增加到0.783 +/- 0.11 g/ cm2(从基线2.91 +/- 2.56%/年变化%)。16例对照组患者骨密度降低(从基线变化百分比1.55 +/- 2.48%)(P < 0.0012)。经替地膦酸钠治疗后,A组骨密度明显高于B组或对照组。A组7例患者6个月时BMD明显增高,但12个月时BMD较6个月时无明显增高。另一方面,8例a组患者在间歇性循环替地酸治疗2年后,骨密度有增加的趋势。替地酸治疗无不良反应,实验室资料未见异常。虽然A组在研究前仅有2例出现压缩性骨折的发现,但在本研究过程中,所有组均未出现新的压缩性骨折。结论:周期性地替膦酸钠治疗类固醇性骨质疏松是有效的。
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[The clinical benefits to bone mineral density were shown by cyclical oral etidronate administration in steroid induced osteoporosis].

Purpose: To compare the bone-mass effects of intermittent cyclic etidronate administration in patients of various rheumatic disease patients with corticosteroid-induced osteoporosis.

Patients and methods: We evaluated bone mineral density (BMD) of lumbar spine in 34 female patients (mean age: 46.4 +/- 13.7 y. o. 17-71) treated with long term corticosteroid (> 6 months). Eighteen patients cyclically received etidronate orally (400 mg or 200 mg etidronate daily for 2 weeks, followed by 10-12 weeks drug-free periods). Twelve in these 18 patients received 400 mg (group A) and another 6 patients were treated with 200 mg/day (group B). Sixteen patients free from etidronate administrations were analysed as a control group.

Results: Cyclical etidronate therapy showed significant increase in BMD. The BMD of lumbar spine increased from 0.760 +/- 0.10 g/cm 2 to 0.783 +/- 0.11 g/cm 2 (%change from baseline 2.91 +/- 2.56%/year) in group A treated patients after 12 months. Reduced BMD (%change from baseline 1.55 +/- 2.48%) was observed in 16 control group patients (P < 0.0012). The BMD in group A was significantly high compared to group B or control after the etidronate treatment. In 7 of group A, BMD increased significantly on 6 months but no more significant increase was shown on 12 months compared to the value on 6 months. On the other hand the BMD tend to increased for after 2 years in intermittent cyclic etidronate treatment in 8 cases of group A. There were no adverse effects and abnormal laboratory data related to the administration of etidronate. Although only 2 cases of group A showed the findings of compression fracture before the study, but no new compression fracture appeared in any group during this study.

Conclusion: It was shown that cyclical etidronate therapy is effective for steroid induced osteoporosis.

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