有不同骨质疏松症用药史女性的持续用药及换药模式:美国 POSSIBLE 研究的 12 个月结果
Persistence and switching patterns among women with varied osteoporosis medication histories: 12-month results from POSSIBLE US.
作者信息
Tosteson A N A, Do T P, Wade S W, Anthony M S, Downs R W
机构信息
HB 7505 Clinical Research, Dartmouth Medical School, 1 Medical Center Drive, Lebanon, NH 03756, USA.
出版信息
Osteoporos Int. 2010 Oct;21(10):1769-80. doi: 10.1007/s00198-009-1133-5. Epub 2010 Jan 26.
UNLABELLED
During the first year of Prospective Observational Scientific Study Investigating Bone Loss Experience (POSSIBE US), many women transitioned (i.e., discontinued or switched) from their baseline osteoporosis medication. Participants not on stable therapy at entry, with side effects, and with poor physical status were at higher risk of transitioning. Understanding factors associated with persistence may lead to improved outcomes.
INTRODUCTION
Postmenopausal osteoporosis (PMO) medication use patterns may differ by treatment history and drug class. We describe these patterns among patients in primary care settings using patient-reported data.
METHODS
Data from 3,006 participants of the POSSIBLE US were used to estimate the probability of a baseline PMO medication transition (i.e., discontinuation or switch) and hazard ratios (HRs) for predictors of these transitions.
RESULTS
One year after study entry, the probability of persisting with a baseline medication was 66% (95% CI: 64-68%). After adjusting for age and osteoporosis diagnosis, factors at entry independently associated with a higher risk of baseline medication transition were treatment status cohort, side effect severity, and OPAQ-SV physical function score. Compared to participants stable on therapy at entry, others had a higher risk, ranging from HR = 1.59 (95% CI: 1.36-1.85) for those new to therapy to HR = 2.00 (95% CI: 1.27-3.15) for those who recently augmented therapy at entry. Participants reporting moderate (HR = 1.31, 95% CI: 1.09-1.57) or severe (HR = 1.88, 95% CI: 1.49-2.39) side effects had a higher risk than those not reporting side effects. Participants reporting Osteoporosis Assessment Questionnaire-Short Version physical function scores in the lowest tertile had a higher risk (HR = 1.27, 95% CI: 1.07-1.52) than those reporting scores in the highest tertile.
CONCLUSION
Baseline osteoporosis medication transitions were common in the first year of POSSIBLE US. Participants not on stable therapy at entry, or who reported severe side effects, or had poor physical health status were at higher risk for these transitions.
未标注
在“前瞻性观察性科学研究调查骨质流失经历(美国POSSIBLE研究)”的第一年,许多女性从其基线骨质疏松症药物治疗方案中转换(即停药或换药)。入组时未接受稳定治疗、有副作用以及身体状况较差的参与者转换治疗方案的风险更高。了解与持续治疗相关的因素可能会改善治疗结果。
引言
绝经后骨质疏松症(PMO)的药物使用模式可能因治疗史和药物类别而异。我们使用患者报告的数据描述基层医疗环境中患者的这些模式。
方法
来自美国POSSIBLE研究的3006名参与者的数据用于估计基线PMO药物治疗方案转换(即停药或换药)的概率以及这些转换预测因素的风险比(HRs)。
结果
入组研究一年后,持续使用基线药物治疗方案的概率为66%(95%置信区间:64 - 68%)。在调整年龄和骨质疏松症诊断后,入组时与基线药物治疗方案转换风险较高独立相关的因素包括治疗状态队列、副作用严重程度和OPAQ - SV身体功能评分。与入组时治疗稳定的参与者相比,其他参与者风险更高,从新开始治疗的参与者的HR = 1.59(95%置信区间:1.36 - 1.85)到入组时最近增加治疗的参与者的HR = 2.00(95%置信区间:1.27 - 3.15)。报告有中度(HR = 1.31,95%置信区间:1.09 - 1.57)或重度(HR = 1.88,95%置信区间:1.49 - 2.39)副作用的参与者比未报告副作用的参与者风险更高。报告骨质疏松症评估问卷简版身体功能评分处于最低三分位数的参与者比报告评分处于最高三分位数的参与者风险更高(HR = 1.27,95%置信区间:1.07 - 1.52)。
结论
在美国POSSIBLE研究的第一年,基线骨质疏松症药物治疗方案转换很常见。入组时未接受稳定治疗、或报告有严重副作用、或身体健康状况较差的参与者发生这些转换的风险更高。
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