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首页> 外文期刊>Patient Preference and Adherence >Comparison of adherence and persistence among multiple sclerosis patients treated with disease-modifying therapies: a retrospective administrative claims analysis
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Comparison of adherence and persistence among multiple sclerosis patients treated with disease-modifying therapies: a retrospective administrative claims analysis

机译:疾病改变疗法治疗的多发性硬化症患者依从性和持久性的比较:回顾性行政要求分析

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Purpose: To compare adherence and persistence among patients with multiple sclerosis (MS) initiated on disease-modifying therapy (DMTs), including intramuscular (IM) interferon beta-1a (IFNβ-1a), subcutaneous (SC) IFNβ-1a, IFNβ-1b, or glatiramer acetate (GA).Methods: MS patients initiated on IM-IFNβ-1a, SC-IFNβ-1a, IFNβ-1b, or GA between January 1, 2000 and January 2, 2008 were identified from a retrospective claims database study associated with a large US health plan. The date of DMT initiation was the index date; patients were observed for 6 months before and 12–36 months after the index date. Adherence to the index DMT was measured with a medication possession ratio (MPR), the proportion of days patients possessed their index DMTs; MPR ≥0.80 was considered adherent. Persistence was time in days from index date until the earlier of a minimum 60-day gap in DMT therapy or the last DMT claim during follow-up. Adherence and persistence were modeled with logistic and Cox proportional hazard regressions, respectively.Results: The study population comprised 6,680 patients in the DMT cohorts: IM-IFNβ-1a (N = 2,305, 34.5%); IFNβ-1b (N = 894, 13.4%); GA (N = 2,270, 34.0%); and SC-IFNβ-1a (N = 1,211, 18.1%). The IM-IFNβ-1a cohort had significantly higher regression-adjusted odds of adherence relative to the other cohorts: 52.4% higher odds versus the IFNβ-1b cohort (OR = 0.656, CI = 0.561–0.768); 33.5% higher odds versus the GA cohort (OR = 0.749, CI = 0.665–0.844); and 20.6% higher odds versus the SC-IFNβ-1a cohort (OR = 0.829, CI = 0.719–0.957). There were no consistent differences in persistence between the cohorts.Conclusion: IM-IFNβ-1a patients had significantly higher odds of adherence compared with other DMT cohorts, possibly attributable to IM-IFNβ-1a’s less frequent dosing schedule. The benefits of adherence may include better quality of life, lower risk of relapse, and fewer hospitalizations and emergency visits, making adherence a critical component of MS management.
机译:目的:比较疾病改善疗法(DMT)引发的多发性硬化症(MS)患者的依从性和持久性,包括肌内(IM)干扰素β-1a(IFNβ-1a),皮下(SC)IFNβ-1a,IFNβ-方法:从回顾性索赔数据库中确定2000年1月1日至2008年1月2日之间使用IM-IFNβ-1a,SC-IFNβ-1a,IFNβ-1b或GA引发的MS患者。与一项大型美国卫生计划相关的研究。 DMT启动的日期为索引日期;在索引日期之前和之后的12–36个月内观察患者。用药物拥有率(MPR)衡量患者对指数DMT的依从性,即患者拥有指数DMT的天数。 MPR≥0.80被认为是依从性的。持续时间是指从索引日期算起,直到DMT治疗至少间隔60天或随访期间最后一次DMT索赔中较早者的时间。结果:研究人群包括6,680例DMT队列:IM-IFNβ-1a(N = 2,305,34.5%);依从性和持久性分别用logistic和Cox比例风险回归建模。 IFNβ-1b(N = 894,13.4%); GA(N = 2,270,34.0%);和SC-IFNβ-1a(N = 1,211,18.1%)。与其他队列相比,IM-IFNβ-1a队列的回归调整依从性显着更高:与IFNβ-1b队列相比,IM-IFNβ-1a队列的依从性概率高52.4%(OR = 0.656,CI = 0.561–0.768);与GA队列相比,胜算率高33.5%(OR = 0.749,CI = 0.665-0.844);与SC-IFNβ-1a组相比,机率高出20.6%(OR = 0.829,CI = 0.719-0.957)。结论:IM-IFNβ-1a患者的依从性比其他DMT人群显着更高,可能归因于IM-IFNβ-1a的给药频率较低。坚持治疗的好处可能包括改善生活质量,降低复发风险,减少住院和急诊就诊,这使坚持治疗成为MS管理的重要组成部分。

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