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低剂量静脉注射3-氨基-1-羟基亚丙基-1,1-二膦酸盐(APD)治疗骨Paget病。

Low dose intravenous 3-amino-1-hydroxypropylidene-1,1-bisphosphonate (APD) for the treatment of Paget's disease of bone.

作者信息

Cantrill J A, Buckler H M, Anderson D C

出版信息

Ann Rheum Dis. 1986 Dec;45(12):1012-8. doi: 10.1136/ard.45.12.1012.

Abstract

Twenty patients with severe symptomatic Paget's disease were treated with a series of 15 mg intravenous infusions of 3-amino-1-hydroxypropylidene-1,1-bisphosphonate (APD). A regimen of either five consecutive days of treatment (regimen 1) or a course of 12 weekly infusions was administered (regimen 2). In five cases regimen 2 followed regimen 1 after a three month interval. Alkaline phosphatase levels fell in all patients and returned to the normal range in 12. All but one of the patients obtained symptomatic improvement. There was a median fall in alkaline phosphatase activity of 63%. Eight patients observed a transient increase in bone pain starting about 24 hours after the first infusion. Intravenous APD was well tolerated, and we conclude that it is an effective treatment for Paget's disease; this route of administration avoids the problem of poor and unpredictable gastrointestinal absorption seen when a bisphosphonate is given orally. The optimal dose and duration of APD therapy, frequency of relapse, requirement for further courses, and merits relative to other second generation bisphosphonates remain to be established.

摘要

20例有严重症状的佩吉特病患者接受了一系列15毫克静脉输注3-氨基-1-羟基亚丙基-1,1-二膦酸盐(APD)的治疗。采用连续5天治疗方案(方案1)或12周每周输注一次的疗程(方案2)。5例患者在间隔3个月后采用方案2继方案1进行治疗。所有患者的碱性磷酸酶水平均下降,12例恢复到正常范围。除1例患者外,所有患者症状均有改善。碱性磷酸酶活性中位数下降63%。8例患者在首次输注后约24小时开始出现骨痛短暂加重。静脉输注APD耐受性良好,我们得出结论,它是治疗佩吉特病的有效方法;这种给药途径避免了口服双膦酸盐时出现的胃肠道吸收差且不可预测的问题。APD治疗的最佳剂量和疗程、复发频率、进一步疗程的需求以及相对于其他第二代双膦酸盐的优点仍有待确定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4c9f/1002042/7390a9b9cc7b/annrheumd00279-0048-a.jpg

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