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首页> 外文期刊>Bone >Comparison of risedronate versus placebo in preventing anastrozole-induced bone loss in women at high risk of developing breast cancer with osteopenia
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Comparison of risedronate versus placebo in preventing anastrozole-induced bone loss in women at high risk of developing breast cancer with osteopenia

机译:用骨质脑膜发育乳腺癌患乳腺癌的高危妇女骨质骨质骨质骨质骨丢失

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摘要

Anastrozole has been shown to prevent breast cancer in postmenopausal women at high risk of the disease, but has been associated with substantial accelerated loss of bone mineral density (BMD) and increased fractures. Here, we investigate the effect of risedronate on BMD after 5 years of follow-up in the IBIS-II prevention trial. 1410 women were enrolled in the bone sub-study and stratified into three strata according to the lowest baseline T-score at spine or femoral neck. The objective was to compare the effect of oral risedronate (35 mg weekly) versus placebo in osteopenic women in stratum II who were randomised to anastrozole in the main study. 258 osteopenic, postmenopausal women at high risk of developing breast cancer for whom baseline and follow-up bone mineral density measurements were available. 5-year mean BMD change at the lumbar spine for osteopenic women randomised to anastrozole and risedronate was 0.4% compared to 4.2% for those not on risedronate (P < 0.0001) but not significantly different between risedronate users and non-users at the hip (P = 0.2). 5-year mean PINP change was 20% for those randomised to anastrozole and risedronate compared to 3% for those not on risedronate but on anastrozole (P < 0.0001). Our results confirm the bone loss associated with the use of anastrozole and show that anastrozole-induced BMD loss in the spine can be controlled with risedronate treatment. However, our results suggest that weekly oral risedronate is unable to completely prevent anastrozole induced bone loss at the hip.
机译:Anstrozole已被证明在疾病的高风险中预防绝经后妇女的乳腺癌,但已经与骨矿物密度(BMD)的大量加速丧失和骨折有关。在这里,我们在IBIS-II预防试验中5年后的5年后,我们调查了日出riseNate对BMD的影响。根据脊柱或股骨颈的最低基线T分数,1410名妇女在骨质研究中注册并分为三个层次。该目的是将口中日出型(35毫克每周)对骨瘦如柴妇女在主要研究中随机的骨质妇女中的骨质促进妇女的影响。 258例骨质骨,绝经后妇女患有高风险的乳腺癌,可用于基线和后续骨密度测量的乳腺癌。 5年5年的平均BMD变化对于骨质胸脊柱,随机向Anastrozole和Ristronate患者为0.4%,而不是在Ristronate(P <0.0001)的4.2%(P <0.01),但在臀部的日式用户和非用户之间没有显着差异( p = 0.2)。 5年的平均PINP变化为Anstrozole和Ristronate的那些,而Lowerronate的in 20%,而不是在Ristronate但在Anstrozole上的3%(P <0.0001)。我们的结果证实了与Anstrozole的使用相关的骨质损失,并显示脊柱中的Anstrozole诱导的BMD损失可以用Risedronate治疗来控制。但是,我们的结果表明,每周口中日式炖植物无法完全防止髋关节中的Anstrozole诱导骨质损失。

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