selexipag维持剂量对美国肺动脉高压患者坚持治疗、依从性和住院治疗的影响。

IF 2.2 4区 医学 Q2 CARDIAC & CARDIOVASCULAR SYSTEMS Pulmonary Circulation Pub Date : 2024-08-18 eCollection Date: 2024-07-01 DOI:10.1002/pul2.12415
Charles D Burger, Wenze Tang, Yuen Tsang, Sumeet Panjabi
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引用次数: 0

摘要

Selexipag 是一种口服前列环素受体选择性激动剂,已被批准用于治疗成人肺动脉高压 (PAH)。Selexipag 的初始剂量为 200 微克,每天两次(bid),通常每周滴定 200 微克 bid(按标签)或更缓慢地滴定(例如,在实际临床实践中每隔一周滴定一次),以达到最高耐受个体化剂量(ID),从 200 微克到 1600 微克 bid 不等。在 3 期 GRIPHON 试验中,与安慰剂相比,selexipag 可延缓疾病进展并降低 PAH 相关住院风险;在三个预先指定的个体化剂量组:低剂量组(200-400 µg bid)、中剂量组(600-1000 µg bid)和高剂量组(1200-1600 µg bid)中,效果一致。本研究评估了现实世界中不同selexipag剂量范围的患者疗效。研究分析了来自 Komodo 封闭索赔数据库(2015-2022 年)的 1186 名服用 selexipag 的美国 PAH 成年患者的数据。其中,634 名(53.5%)患者完成滴定并达到了他们的 selexipag ID(43.8% 高 ID,29.8% 中 ID,26.3% 低 ID)。随后,72.4% 的低内径组患者进行了剂量调整,而中内径组为 61.9%,高内径组为 34.5%;标准化平均差为 0.63。不同ID组的患者预后,即持续用药时间(停药时间)以及全因和PAH相关住院风险无明显差异。与 GRIPHON 试验和其他研究结果类似,在这一多样化、真实世界中的 PAH 患者群体中得出的研究结果强化了个体化用药方案,以最大限度地降低获益风险,并使 Selexipag 达到最高耐受剂量。
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Impact of selexipag maintenance dose on persistence, adherence, and hospitalization in US patients with pulmonary arterial hypertension.

Selexipag is an oral selective agonist of the prostacyclin receptor approved to treat adults with pulmonary arterial hypertension (PAH). Selexipag is initiated at a dose of 200 μg twice daily (bid) and usually titrated up by 200 μg bid weekly (per label) or more slowly (e.g., every other week in real-world clinical practice) to the highest tolerated individualized dose (ID) ranging from 200 to 1600 µg bid. In the Phase 3 GRIPHON trial, selexipag delayed disease progression and reduced risk of PAH-related hospitalization compared with placebo; the effect was consistent across three prespecified ID groups: low (200-400 µg bid), medium (600-1000 µg bid), and high (1200-1600 µg bid). This study evaluated patient outcomes across selexipag dose ranges in real-world practice. Data were analyzed from 1186 US adult patients with PAH on selexipag from the Komodo closed-claims database (2015‒2022). Of these, 634 (53.5%) patients completed titration and reached their selexipag ID (43.8% high ID, 29.8% medium ID, 26.3% low ID). Subsequently, 72.4% of patients in the low ID group had dose adjustments compared with 61.9% (medium ID) and 34.5% (high ID; standardized mean difference 0.63). There were no significant differences in patient outcomes, i,e, persistence (time to discontinuation) and risk of all-cause and PAH-related hospitalization across ID groups. The findings in this diverse, real-world population of patients with PAH reinforced an individualized approach to the dosing scheme to maximize benefit-risk and achieve the highest tolerated dose with selexipag similar to findings from the GRIPHON trial and other studies.

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来源期刊
Pulmonary Circulation
Pulmonary Circulation Medicine-Pulmonary and Respiratory Medicine
CiteScore
4.20
自引率
11.50%
发文量
153
审稿时长
15 weeks
期刊介绍: Pulmonary Circulation''s main goal is to encourage basic, translational, and clinical research by investigators, physician-scientists, and clinicans, in the hope of increasing survival rates for pulmonary hypertension and other pulmonary vascular diseases worldwide, and developing new therapeutic approaches for the diseases. Freely available online, Pulmonary Circulation allows diverse knowledge of research, techniques, and case studies to reach a wide readership of specialists in order to improve patient care and treatment outcomes.
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