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与雷洛昔芬和其他骨质疏松症药物使用相关的卒中。

Stroke in relation to use of raloxifene and other drugs against osteoporosis.

机构信息

Department of Endocrinology and Internal Medicine, Aarhus University Hospital, Tage Hansens Gade 2, DK-8000 Arhus C, Denmark.

出版信息

Osteoporos Int. 2011 Apr;22(4):1037-45. doi: 10.1007/s00198-010-1276-4. Epub 2010 May 7.

Abstract

UNLABELLED

Prior studies have associated fatal stroke with raloxifene. In a cohort study, we found no excess risk of stroke with raloxifene; whereas, an excess risk of stroke and fatal stroke was seen with alendronate and etidronate. However, the excess risks were small.

PURPOSE

We aim to study the association between use of raloxifene and other drugs against osteoporosis and risk of stroke.

METHODS

This is a nationwide cohort study from Denmark. All users of bisphosphonates and other drugs against osteoporosis between 1996 and 2006 (n = 103,562) as exposed group and three age- and gender-matched controls from the general population (n = 310,683).

RESULTS

Before the drugs were started, patients later initiating alendronate or raloxifene had fewer strokes than the controls. In contrast, patients who later did start clodronate have more strokes. Among the later users of other bisphosphonates, strontium ranelate or parathyroid hormone, no change in the risk of stroke was present. Patients who started raloxifene neither had an excess risk of strokes nor of fatal strokes. No dose-response relationship was present. Among users of alendronate, a decreasing overall risk of stroke was seen with increasing dose. However, for fatal strokes, the risk increased with increasing dose of alendronate. Among users of etidronate, no trend with dose was present for overall stroke risk; whereas for fatal strokes, an increasing risk was seen with increasing dose of etidronate.

CONCLUSIONS

Raloxifene does not seem associated with an excess risk of strokes. The increase seen for alendronate did not seem to be causal as no classical dose-response relationship was present. The dose-response relationship for fatal strokes with alendronate and etidronate needs further examination. However, the excess risks were small and may be due to the underlying disease.

摘要

目的

研究使用雷洛昔芬和其他骨质疏松症治疗药物与中风风险之间的关系。

方法

这是一项来自丹麦的全国性队列研究。将 1996 年至 2006 年期间使用双膦酸盐和其他骨质疏松症治疗药物的所有患者(n=103562)作为暴露组,并从一般人群中匹配年龄和性别相同的 310683 名患者作为对照组。

结果

在开始使用药物之前,后来开始使用阿伦膦酸盐或雷洛昔芬的患者发生中风的次数少于对照组。相比之下,后来开始使用氯屈膦酸盐的患者中风次数更多。在后来使用其他双膦酸盐、锶雷尼酸或甲状旁腺激素的患者中,中风风险没有变化。开始使用雷洛昔芬的患者既没有中风风险增加,也没有致命性中风风险增加。未发现剂量反应关系。在使用阿伦膦酸盐的患者中,随着剂量的增加,总体中风风险呈下降趋势。然而,对于致命性中风,随着阿伦膦酸盐剂量的增加,风险增加。在使用依替膦酸盐的患者中,总体中风风险与剂量之间没有趋势;然而,致命性中风的风险随着依替膦酸盐剂量的增加而增加。

结论

雷洛昔芬似乎与中风风险增加无关。阿伦膦酸盐的增加似乎不是因果关系,因为没有明显的剂量反应关系。需要进一步研究阿伦膦酸盐和依替膦酸盐与致命性中风之间的剂量反应关系。然而,风险增加幅度较小,可能是由于潜在疾病所致。

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