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Treatment Discontinuation and Disease Progression with Injectable Disease-Modifying Therapies

机译:注射性疾病改良疗法的治疗中止和疾病进展

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Injectable first-line disease-modifying therapies (DMTs) for multiple sclerosis (MS) are generally prescribed for continuous use. Accordingly, the various factors that influence patient persistence with treatment and that can lead some patients to switch medications or discontinue treatment may affect clinical outcomes. Using data from the North American Research Committee on Multiple Sclerosis (NARCOMS) database, this study evaluated participants` reasons for discontinuation of injectable DMTs as well as the relationship between staying on therapy and sustained patient-reported disease progression and annualized relapse rates. Participants selected their reason(s) for discontinuation from among 16 possible options covering the categories of efficacy, safety, tolerability, and burden, with multiple responses permitted. Both unadjusted data and data adjusted for baseline age, disease duration, disability, and sex were evaluated. Discontinuation profiles varied among DMTs. Participants on intramuscular interferon beta-1a (IM IFNβ-1a) and glatiramer acetate (GA) reported the fewest discontinuations based on safety concerns, although GA was associated with reports of higher burden and lower efficacy than other therapies. Difficulties with tolerability were more often reported as a reason for discontinuing subcutaneous (SC) IFNβ-1a than as a reason for discontinuing IM IFNβ-1a, GA, or SC IFNβ-1b. In the persistent therapy cohort, less patient-reported disability progression was reported with IM IFNβ-1a treatment than with SC IFNβ-1a, IFNβ-1b, or GA. These findings have relevance to clinical decision making and medication compliance in MS patient care.
机译:通常规定用于多发性硬化症(MS)的可注射的一线疾病缓解疗法(DMT)可连续使用。因此,影响患者坚持治疗并导致某些患者改用药物或中止治疗的各种因素可能会影响临床结果。使用来自北美多发性硬化症研究委员会(NARCOMS)数据库的数据,本研究评估了参与者停用可注射DMT的原因,以及坚持治疗与患者报告的持续疾病进展和年复发率之间的关系。参加者从16种可能的选择中选择了停药的原因,这些选择涉及功效,安全性,耐受性和负担类别,并允许做出多种反应。评估未调整数据和针对基线年龄,疾病持续时间,残疾和性别调整的数据。 DMT的停产情况有所不同。尽管出于安全考虑,肌注干扰素β-1a(IMIFNβ-1a)和醋酸格拉替雷(GA)的参与者报告的停药最少,尽管与其他疗法相比,GA与更高的负担和更低的疗效有关。与耐受性有关的困难更多地被报道为中止皮下(SC)IFNβ-1a的原因,而非中止IMIFNβ-1a,GA或SCIFNβ-1b的原因。在持续治疗队列中,IMIFNβ-1a治疗的患者报告的残疾进展少于SCIFNβ-1a,IFNβ-1b或GA。这些发现与MS患者护理中的临床决策和药物依从性有关。

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