Lo J C, Pressman A R, Omar M A, Ettinger B
Division of Research, Kaiser Permanente Northern California, 2000 Broadway, Oakland, CA 94612, USA.
Osteoporos Int. 2006;17(6):922-8. doi: 10.1007/s00198-006-0085-2. Epub 2006 Apr 12.
Although clinical trials indicate that oral bisphosphonates reduce osteoporotic fracture risk, compliance with bisphosphonate therapy in practice is suboptimal, with 1-year discontinuation rates exceeding 50%.
We conducted a retrospective cohort study among female members of a large integrated health care delivery system (Kaiser Permanente of Northern California), age 45 years and older, to determine their persistence with weekly alendronate (defined as continuous use, allowing for a refill gap of 60 days), predictors of discontinuation, and subsequent osteoporosis therapy. We also examined the effect of varying the refill gap from 30 to 120 days on the discontinuation rate. From 2002 through 2003, we identified 13,455 women (age 68.8+/-10.4 years) who initiated weekly oral alendronate therapy.
Using a 60-day refill gap, the 1-year discontinuation rate was 49.6% [95% confidence interval (CI) 48.8-50.4%]; this increased to 58.0% (CI 57.2-58.8%) with a 30-day gap and decreased to 42.2% (CI 41.1-43.0%) with a 120-day gap. Among those who discontinued therapy, about one-third restarted alendronate or another osteoporosis drug within 6 months. Baseline factors associated with alendronate discontinuation included prior bone mineral density testing [adjusted odds ratio (OR) 0.64, CI 0.60-0.69], prior postmenopausal hormone therapy (OR 0.78, CI 0.73-0.84), prior high-dose oral glucocorticoid therapy (OR 1.26, CI 1.05-1.51), prior gastrointestinal diagnoses (OR 1.21, CI 1.09-1.36), and high number of therapeutic classes of prescriptions filled in the prior year (OR 1.21, CI 1.10-1.32), although the final model had limited explanatory power.
We conclude that apparent discontinuation rates are high within 1 year after treatment initiation, although a subset of women appears to restart bisphosphonate or other osteoporosis therapy. Because intermittent use and/or poor adherence is common, discontinuation rates based on data from administrative databases are sensitive to the refill gap length. In addition, we identified no clinical factors highly predictive of discontinuation.
尽管临床试验表明口服双膦酸盐可降低骨质疏松性骨折风险,但在实际应用中,双膦酸盐治疗的依从性并不理想,1年停药率超过50%。
我们对一个大型综合医疗保健系统(北加利福尼亚州凯撒医疗集团)中45岁及以上的女性成员进行了一项回顾性队列研究,以确定她们持续使用每周一次阿仑膦酸钠的情况(定义为持续使用,允许有60天的再填充间隔)、停药的预测因素以及后续的骨质疏松治疗。我们还研究了将再填充间隔从30天调整到120天对停药率的影响。从2002年到2003年,我们确定了13455名开始每周口服阿仑膦酸钠治疗的女性(年龄68.8±10.4岁)。
使用60天的再填充间隔时,1年停药率为49.6%[95%置信区间(CI)48.8 - 50.4%];30天间隔时增至58.0%(CI 57.2 - 58.8%),120天间隔时降至42.2%(CI 41.1 - 43.0%)。在停药的患者中,约三分之一在6个月内重新开始使用阿仑膦酸钠或其他骨质疏松药物。与阿仑膦酸钠停药相关的基线因素包括既往骨密度检测[调整后的优势比(OR)0.64,CI 0.60 - 0.69]、既往绝经后激素治疗(OR 0.78,CI 0.73 - 0.84)、既往高剂量口服糖皮质激素治疗(OR 1.26,CI 1.05 - 1.51)、既往胃肠道疾病诊断(OR 1.21,CI 1.09 - 1.36)以及前一年开具的治疗类别处方数量较多(OR 1.21,CI 1.10 - 1.32),尽管最终模型的解释力有限。
我们得出结论,治疗开始后1年内的明显停药率较高,尽管有一部分女性似乎会重新开始双膦酸盐或其他骨质疏松治疗。由于间歇使用和/或依从性差很常见,基于行政数据库数据的停药率对再填充间隔长度很敏感。此外,我们未发现高度预测停药的临床因素。
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