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唑来膦酸首次给药时间与髋部骨折后抗骨折疗效及死亡率降低的关系

Antifracture efficacy and reduction of mortality in relation to timing of the first dose of zoledronic acid after hip fracture.

作者信息

Eriksen Erik Fink, Lyles Kenneth W, Colón-Emeric Cathleen S, Pieper Carl F, Magaziner Jay S, Adachi Jonathan D, Hyldstrup Lars, Recknor Chris, Nordsletten Lars, Lavecchia Catherine, Hu Huilin, Boonen Steven, Mesenbrink Peter

机构信息

Novartis Pharma, Basel, Switzerland.

出版信息

J Bone Miner Res. 2009 Jul;24(7):1308-13. doi: 10.1359/jbmr.090209.

Abstract

Annual infusions of zoledronic acid (5 mg) significantly reduced the risk of vertebral, hip, and nonvertebral fractures in a study of postmenopausal women with osteoporosis and significantly reduced clinical fractures and all-cause mortality in another study of women and men who had recently undergone surgical repair of hip fracture. In this analysis, we examined whether timing of the first infusion of zoledronic acid study drug after hip fracture repair influenced the antifracture efficacy and mortality benefit observed in the study. A total of 2127 patients (1065 on active treatment and 1062 on placebo; mean age, 75 yr; 76% women and 24% men) were administered zoledronic acid or placebo within 90 days after surgical repair of an osteoporotic hip fracture and annually thereafter, with a median follow-up time of 1.9 yr. Median time to first dose after the incident hip fracture surgery was approximately 6 wk. Posthoc analyses were performed by dividing the study population into 2-wk intervals (calculated from time of first infusion in relation to surgical repair) to examine effects on BMD, fracture, and mortality. Analysis by 2-wk intervals showed a significant total hip BMD response and a consistent reduction of overall clinical fractures and mortality in patients receiving the first dose 2-wk or later after surgical repair. Clinical fracture subgroups (vertebral, nonvertebral, and hip) were also reduced, albeit with more variation and 95% CIs crossing 1 at most time points. We concluded that administration of zoledronic acid to patients suffering a low-trauma hip fracture 2 wk or later after surgical repair increases hip BMD, induces significant reductions in the risk of subsequent clinical vertebral, nonvertebral, and hip fractures, and reduces mortality.

摘要

在一项针对绝经后骨质疏松症女性的研究中,每年输注唑来膦酸(5毫克)可显著降低椎体、髋部和非椎体骨折的风险;在另一项针对近期接受髋部骨折手术修复的女性和男性的研究中,每年输注唑来膦酸可显著降低临床骨折风险和全因死亡率。在本分析中,我们研究了髋部骨折修复后首次输注唑来膦酸研究药物的时间是否会影响研究中观察到的抗骨折疗效和死亡率获益。共有2127例患者(1065例接受活性治疗,1062例接受安慰剂;平均年龄75岁;女性占76%,男性占24%)在骨质疏松性髋部骨折手术修复后90天内接受唑来膦酸或安慰剂治疗,此后每年一次,中位随访时间为1.9年。首次髋部骨折手术后至首次给药的中位时间约为6周。通过将研究人群按2周间隔(从首次输注时间相对于手术修复时间计算)进行分组进行事后分析,以检查对骨密度、骨折和死亡率的影响。按2周间隔分析显示,在手术修复后2周或更晚接受首次剂量的患者中,全髋骨密度有显著反应,总体临床骨折和死亡率持续降低。临床骨折亚组(椎体、非椎体和髋部)也有所减少,尽管在大多数时间点变化更大且95%置信区间最多有一个交叉点为1。我们得出结论,在手术修复后2周或更晚对低创伤性髋部骨折患者给予唑来膦酸可增加髋部骨密度,显著降低随后临床椎体、非椎体和髋部骨折的风险,并降低死亡率。

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