非佐利奈坦治疗绝经相关中重度血管舒缩症状:两项 3 期研究(SKYLIGHT 1 和 2)中内在和外在因素的影响。
Fezolinetant treatment of moderate-to-severe vasomotor symptoms due to menopause: effect of intrinsic and extrinsic factors in two phase 3 studies (SKYLIGHT 1 and 2).
机构信息
From the Department of Obstetrics and Gynecology, University of Colorado School of Medicine, Aurora, CO.
Department of Obstetrics & Gynecology, UNC School of Medicine, Chapel Hill, NC.
出版信息
Menopause. 2024 Apr 1;31(4):247-257. doi: 10.1097/GME.0000000000002340.
OBJECTIVE
This study aimed to assess the efficacy of the neurokinin 3 receptor antagonist, fezolinetant, according to several intrinsic (individual related) and extrinsic (external influence) factors that may influence the frequency and severity of moderate-to-severe vasomotor symptoms (VMS) using pooled 12-week data from SKYLIGHT 1 and 2.
METHODS
SKYLIGHT 1 and 2 were two phase 3, randomized, double-blind studies conducted from July 2019 to August 2021 (SKYLIGHT 1) or April 2021 (SKYLIGHT 2). Participants were initially randomized to receive daily doses of placebo, fezolinetant 30 mg, or fezolinetant 45 mg. After 12 weeks, placebo participants were rerandomized to receive fezolinetant 30 mg or 45 mg, whereas those receiving fezolinetant continued on the same dose. Change in VMS frequency from baseline to week 12 was used to assess efficacy according to several intrinsic and extrinsic factors. Overall efficacy and safety were also investigated.
RESULTS
Overall, 1,022 individuals were included. Fezolinetant was efficacious in reducing VMS frequency across all intrinsic and extrinsic factors. Efficacy was most notable for participants who self-identify as Black (least squares mean difference for fezolinetant 45 mg versus placebo, -3.67; 95% CI, -5.32 to -2.01), current smokers (-3.48; -5.19 to -1.77), and current alcohol users (-3.48; -4.42 to -2.54). Overall efficacy was -2.51 (95% CI, -3.20 to -1.82) for fezolinetant 45 mg versus placebo. Similar findings were observed for the fezolinetant 30 mg dose. Comparable incidences of treatment-emergent adverse events were observed for placebo (132 of 342 individuals [38.6%]), fezolinetant 30 mg (132 of 340 individuals [38.8%]), and fezolinetant 45 mg (135 of 340 individuals [39.7%]).
CONCLUSIONS
None of the intrinsic and extrinsic factors analyzed substantially reduced the efficacy response to fezolinetant in SKYLIGHT 1 and 2. These data provide additional confidence for using fezolinetant in a diverse population of individuals with VMS.
目的
本研究旨在根据可能影响中重度血管舒缩症状(VMS)频率和严重程度的几个内在(个体相关)和外在(外部影响)因素,评估神经激肽 3 受体拮抗剂 fezolinetant 的疗效。这是使用 SKYLIGHT 1 和 2 的 12 周汇总数据得出的结果。
方法
SKYLIGHT 1 和 2 是两项 3 期、随机、双盲研究,分别于 2019 年 7 月至 2021 年 8 月(SKYLIGHT 1)或 2021 年 4 月(SKYLIGHT 2)进行。参与者最初被随机分配接受安慰剂、fezolinetant 30mg 或 fezolinetant 45mg 的每日剂量。12 周后,安慰剂组参与者被重新随机分配接受 fezolinetant 30mg 或 45mg,而接受 fezolinetant 的参与者继续接受相同剂量。根据几个内在和外在因素,使用 VMS 频率从基线到 12 周的变化来评估疗效。还调查了整体疗效和安全性。
结果
总体而言,共有 1022 人入组。在所有内在和外在因素下,fezolinetant 均能有效降低 VMS 频率。对于自我认定为黑人的参与者(fezolinetant 45mg 与安慰剂相比的最小二乘均值差异,-3.67;95%CI,-5.32 至-2.01)、当前吸烟者(-3.48;-5.19 至-1.77)和当前饮酒者(-3.48;-4.42 至-2.54),疗效最为显著。与安慰剂相比,fezolinetant 45mg 的总体疗效为-2.51(95%CI,-3.20 至-1.82)。对于 fezolinetant 30mg 剂量,也观察到了类似的疗效。安慰剂(342 人中有 132 人[38.6%])、fezolinetant 30mg(340 人中有 132 人[38.8%])和 fezolinetant 45mg(340 人中有 135 人[39.7%])的治疗中出现的不良事件发生率相当。
结论
在 SKYLIGHT 1 和 2 中,没有任何内在和外在因素显著降低了 fezolinetant 的疗效反应。这些数据为在 VMS 患者的多样化人群中使用 fezolinetant 提供了更多信心。
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