Effect of fezolinetant on sleep disturbance and impairment during treatment of vasomotor symptoms due to menopause

IF 3.9 2区医学 Q2 GERIATRICS & GERONTOLOGY Maturitas Pub Date : 2024-05-15 DOI:10.1016/j.maturitas.2024.107999

Marla Shapiro C.M. , Antonio Cano , Rossella E. Nappi , Nanette Santoro , Marci L. English , Shayna Mancuso , Antonia Morga , Emad Siddiqui , Udaya Valluri , Faith D. Ottery

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Abstract

Objectives

To analyse the effect of fezolinetant on patient-reported sleep disturbance and impairment in individuals with vasomotor symptoms (VMS) using pooled data from the SKYLIGHT 1 and 2 studies.

Study design

The SKYLIGHT studies were phase-3, double-blind investigations. Individuals (≥40–≤65 years) who were assigned female at birth and seeking treatment of/relief from moderate-to-severe VMS were enrolled. Participants were randomised to receive placebo, fezolinetant 30 mg, or fezolinetant 45 mg during a 12-week treatment period.

Main outcome measures

Sleep assessments: Patient-Reported Outcomes Measurement Information System Sleep Disturbance – Short Form 8b (PROMIS SD SF 8b), PROMIS Sleep-Related Impairment – Short Form 8a (PROMIS SRI SF 8a), and Patient Global Impression of Change/Severity in SD (PGI-C SD and PGI-S SD). Assessments were completed at baseline (except PGI-C SD), weeks 4 and 12.

Results

Overall, 1022 individuals were randomised and took ≥1 dose of study drug. PROMIS SD SF 8b results showed that improvements in sleep disturbance were observed for fezolinetant 30 and 45 mg versus placebo (week 12, least squares [LS] mean differences: −0.6 [95 % confidence interval [CI]: −1.7, 0.4] for 30 mg and –1.5 [−2.5, −0.5] for 45 mg). Similar improvements in sleep impairment were reported using the PROMIS SRI SF 8a (week 12, LS mean differences: –1.1 [95 % CI: −2.1, −0.1] for 30 mg and −1.3 [−2.3, −0.3] for 45 mg). For PGI-C SD at week 12, 33.6 % (98/292 participants) of the placebo group felt much/moderately better versus 40.1 % (110/274) and 51.0 % (154/302) of the fezolinetant 30 mg and 45 mg groups, respectively. For PGI-S SD at week 12, 44.0 % (129/293) of the placebo group had severe/moderate problems versus 41.1 % (113/275) and 36.6 % (111/303) of the fezolinetant 30 mg and 45 mg groups, respectively. The 12-week timeframe for this analysis was limited by the length of the placebo-controlled period.

Conclusions

Fezolinetant had a beneficial effect on four measures of sleep disturbance and impairment following treatment for VMS.

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非唑烷酮对治疗更年期血管运动症状期间睡眠障碍的影响。

研究目的利用SKYLIGHT 1和2研究的汇总数据，分析非佐利奈坦对血管运动症状（VMS）患者报告的睡眠障碍和损伤的影响：SKYLIGHT研究为第三阶段双盲研究。研究对象为出生时即被指定为女性、寻求治疗/缓解中度至重度VMS的患者（≥40-≤65岁）。在为期12周的治疗期间，参与者被随机分配接受安慰剂、非佐林内酯30毫克或非佐林内酯45毫克的治疗：睡眠评估：主要结果指标：睡眠评估：患者报告结果测量信息系统睡眠障碍--简表8b（PROMIS SD SF 8b）、PROMIS睡眠相关损害--简表8a（PROMIS SRI SF 8a）和患者对SD变化/严重程度的总体印象（PGI-C SD和PGI-S SD）。评估在基线（PGI-C SD除外）、第4周和第12周完成：共有 1022 人接受了随机治疗，并服用了≥1 剂研究药物。PROMIS SD SF 8b 结果显示，非索内酯 30 毫克和 45 毫克与安慰剂相比，睡眠障碍有所改善（第 12 周，最小二乘法 [LS] 平均差：-0.6 [95 % 置信度]）：30毫克为-0.6[95%置信区间[CI]：-1.7，0.4]，45毫克为-1.5[-2.5，-0.5]）。使用 PROMIS SRI SF 8a 对睡眠障碍也有类似的改善（第 12 周，LS 平均差异：-1.1 [95 % 置信区间 [CI]：-2.5 [-0.530毫克为-1.1 [95 % CI：-2.1, -0.1]，45毫克为-1.3 [-2.3, -0.3]）。在第 12 周的 PGI-C SD 方面，安慰剂组有 33.6%（98/292 名参与者）的人感觉好得多/中等程度，而非唑内酯 30 毫克组和 45 毫克组分别有 40.1%（110/274 名参与者）和 51.0%（154/302 名参与者）的人感觉好得多/中等程度。至于第 12 周的 PGI-S SD，安慰剂组中 44.0%（129/293）的患者有严重/中度问题，而非唑仑内酯 30 毫克组和 45 毫克组分别为 41.1%（113/275）和 36.6%（111/303）。由于安慰剂对照期的长度限制，本次分析的时间范围为12周：结论：非佐林内酯对VMS治疗后睡眠障碍的四项指标均有益处。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Maturitas 医学-妇产科学

CiteScore

9.10

自引率

2.00%

发文量

142

审稿时长

40 days

期刊介绍： Maturitas is an international multidisciplinary peer reviewed scientific journal of midlife health and beyond publishing original research, reviews, consensus statements and guidelines, and mini-reviews. The journal provides a forum for all aspects of postreproductive health in both genders ranging from basic science to health and social care. Topic areas include:• Aging• Alternative and Complementary medicines• Arthritis and Bone Health• Cancer• Cardiovascular Health• Cognitive and Physical Functioning• Epidemiology, health and social care• Gynecology/ Reproductive Endocrinology• Nutrition/ Obesity Diabetes/ Metabolic Syndrome• Menopause, Ovarian Aging• Mental Health• Pharmacology• Sexuality• Quality of Life