Fractures after Initiation of a Drug Holiday in a Real- Life Setting

Michael Morkos, Sanford Baim, Alessandra Casagrande, Paul Mahrous, Muriel Tania L Go, Hasan Husni, Mirette Hanna, Sara Bedrose, Dingfeng Li
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Abstract

Purpose: We aimed to assess the fracture rate in patients who were placed on a drug holiday (DH) after minimum adequate therapy versus those who continued therapy (CT) in a real-life setting. Methods: This is a retrospective cohort study conducted in a tertiary academic center. Inclusion criteria involved osteoporotic adults who received minimum adequate bisphosphonate therapy (≥ 3 years), otherwise, patients were excluded. Results: Of 1,814 charts randomly selected and reviewed, 272 patients met the inclusion criteria. In our cohort, females were 90.9%, White 50.0%, and African American 40.5%. A DH was initiated in 119 patients (43.8%). In the CT versus DH cohorts, the mean duration of therapy was 6.0 ± 2.6 versus 5.7 ± 2.3 years, total duration of follow-up 6.9 ± 2.9 versus 7.8 ± 2.7 years, and fractures occurred in 11.7% versus 9.2% respectively, not statistically different. The mean duration of follow-up after starting DH was 2.5 ± 1.9 years. Upon risk stratification using FRAX scoring, in the high-risk cohort, fragility fractures occurred in 16.5% (n=22/133) of the CT group versus 13.5% (n=7/52) of the DH cohort (P=0.66). In the lower risk cohort based on FRAX scoring, fragility fractures occurred in 7.1% (n=10/131) of the CT group versus 6.0% (n=4/63) of the DH cohort (P=1.0). Conclusion: In our cohort, continued drug therapy did not provide additional fracture protective benefits beyond the minimum adequate duration of therapy. A drug holiday after three to five years of treatment may be considered after review of risk factors for future fracture.
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在现实生活中开始药物假期后的骨折
目的:我们的目的是评估在最低限度的适当治疗后被放置在药物假期(DH)的患者与在现实生活中继续治疗(CT)的患者的骨折率。方法:回顾性队列研究,在某高等学术中心进行。纳入标准为骨质疏松的成年人,接受最低限度的足量双膦酸盐治疗(≥3年),否则排除患者。结果:在随机选取的1814份病历中,有272例患者符合纳入标准。在我们的队列中,女性占90.9%,白人占50.0%,非裔美国人占40.5%。119例(43.8%)患者开始接受健康护理。CT组和DH组的平均治疗时间分别为6.0±2.6年和5.7±2.3年,总随访时间分别为6.9±2.9年和7.8±2.7年,骨折发生率分别为11.7%和9.2%,差异无统计学意义。开始DH后的平均随访时间为2.5±1.9年。在使用FRAX评分进行风险分层后,在高危队列中,CT组发生脆性骨折的比例为16.5% (n=22/133),而DH组为13.5% (n=7/52) (P=0.66)。在基于FRAX评分的低风险队列中,CT组脆性骨折发生率为7.1% (n=10/131),而DH组为6.0% (n=4/63) (P=1.0)。结论:在我们的队列中,持续的药物治疗并没有提供额外的骨折保护作用,超过了最小的适当治疗时间。在对未来骨折的危险因素进行评估后,可考虑在治疗3 - 5年后休药。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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