雷洛昔芬对绝经后妇女骨折风险的影响:心脏试验中的雷洛昔芬应用研究
Effects of raloxifene on fracture risk in postmenopausal women: the Raloxifene Use for the Heart Trial.
作者信息
Ensrud Kristine E, Stock John L, Barrett-Connor Elizabeth, Grady Deborah, Mosca Lori, Khaw Kay-Tee, Zhao Qingwen, Agnusdei Donato, Cauley Jane A
机构信息
Center for Chronic Disease Outcomes Research, Veterans Affairs Medical Center, Minneapolis, Minnesota, USA. ensru001@.umn.edu
出版信息
J Bone Miner Res. 2008 Jan;23(1):112-20. doi: 10.1359/jbmr.070904.
UNLABELLED
Using data from a randomized placebo-controlled trial of 10,101 postmenopausal women not selected on the basis of osteoporosis, we examined whether the effect of raloxifene treatment on fractures was consistent across categories of fracture risk. Treatment with raloxifene for 5 yr reduced the risk of clinical vertebral fractures, but not nonvertebral fractures, irrespective of the presence or absence of risk factors for fracture.
INTRODUCTION
In The Raloxifene Use for The Heart (RUTH) trial, women assigned to raloxifene had a lower risk of clinical vertebral fractures but not nonvertebral fractures. However, it is uncertain whether the effect of raloxifene on fractures in this population not selected for low BMD differs according to risk factors for fractures.
MATERIALS AND METHODS
We randomly assigned 10,101 postmenopausal women >or=55 yr of age with documented coronary heart disease or at high risk for coronary events to 60 mg raloxifene daily or placebo and followed them for a median of 5.6 yr. Fractures (nonvertebral and clinical vertebral) were prespecified secondary endpoints that were reported at semiannual visits. Fractures were adjudicated and confirmed using X-ray reports or medical records.
RESULTS
There was no difference between raloxifene and placebo groups in risk of nonvertebral fractures (428 versus 438 events; hazard ratio [HR], 0.96; 95% CI, 0.84-1.10), including hip/femur (89 versus 103 events; HR, 0.85; 95% CI, 0.64-1.13) and wrist (107 versus 111 events; HR, 0.95; 95% CI, 0.73-1.24) fractures. Women treated with raloxifene had a lower risk of clinical vertebral fractures (64 versus 97 events; HR, 0.65; 95% CI, 0.47-0.89). The effect of treatment with raloxifene on risk of nonvertebral and clinical vertebral fractures was consistent across fracture risk categories defined at baseline by age, smoking status, physical activity level, prior history of fracture, family history of hip fracture, diabetes mellitus, previous use of hormone therapy, thyroid hormone use, statin use, weight loss, body mass index, or fracture specific summary risk score.
CONCLUSIONS
In older women with or at high risk of coronary heart disease not selected on the basis of osteoporosis or increased fracture risk, treatment with raloxifene for 5 yr reduced the risk of clinical vertebral fractures, but not nonvertebral fractures, irrespective of presence or absence of risk factors for fracture.
未标注
利用一项针对10101名未基于骨质疏松症进行挑选的绝经后女性的随机安慰剂对照试验的数据,我们研究了雷洛昔芬治疗对骨折的影响在不同骨折风险类别中是否一致。雷洛昔芬治疗5年可降低临床椎体骨折的风险,但对非椎体骨折无此作用,无论是否存在骨折风险因素。
引言
在雷洛昔芬用于心脏(RUTH)试验中,被分配接受雷洛昔芬治疗的女性临床椎体骨折风险较低,但非椎体骨折风险未降低。然而,在这个未因低骨密度而入选的人群中,雷洛昔芬对骨折的影响是否因骨折风险因素而异尚不确定。
材料与方法
我们将10101名年龄≥55岁、有冠心病记录或冠心病事件高危的绝经后女性随机分为每日服用60毫克雷洛昔芬组或安慰剂组,并对她们进行了为期5.6年的中位随访。骨折(非椎体和临床椎体骨折)是预先设定的次要终点,每半年随访时报告。骨折通过X线报告或病历进行判定和确认。
结果
雷洛昔芬组和安慰剂组在非椎体骨折风险方面无差异(分别为428例和438例事件;风险比[HR],0.96;95%置信区间[CI],0.84 - 1.10),包括髋部/股骨骨折(分别为89例和103例事件;HR,0.85;95% CI,0.64 - 1.13)和腕部骨折(分别为107例和111例事件;HR,0.95;95% CI,0.73 - 1.24)。接受雷洛昔芬治疗的女性临床椎体骨折风险较低(分别为64例和97例事件;HR,0.65;95% CI,0.47 - 0.89)。雷洛昔芬治疗对非椎体和临床椎体骨折风险的影响在根据年龄、吸烟状况、身体活动水平、既往骨折史、髋部骨折家族史、糖尿病、既往激素治疗使用情况、甲状腺激素使用情况、他汀类药物使用情况、体重减轻、体重指数或骨折特异性综合风险评分在基线时定义的不同骨折风险类别中是一致的。
结论
在未基于骨质疏松症或骨折风险增加而挑选的患有冠心病或有冠心病高危风险的老年女性中,雷洛昔芬治疗5年可降低临床椎体骨折的风险,但对非椎体骨折无此作用,无论是否存在骨折风险因素。
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