林扎戈利克可迅速减少子宫肌瘤女性的月经过多：PRIMROSE 1和2试验分析

Linzagolix rapidly reduces heavy menstrual bleeding in women with uterine fibroids: an analysis of the PRIMROSE 1 and 2 trials.

作者信息

Donnez Jacques, Becker Christian M, Mangler Mandy, Paszkowski Maciej, Paszkowski Tomasz, St-Pierre Julien, Ionescu-Ittu Raluca, Boolell Mitra, Bestel Elke, Hori Satoshi, Petraglia Felice

机构信息

Société de Recherche pour l'infertilité, Catholic University of Louvain, Brussels, Belgium.

Nuffield Department Women's & Reproductive Health, University of Oxford, Oxford, United Kingdom.

出版信息

Fertil Steril. 2025 Jun;123(6):1093-1100. doi: 10.1016/j.fertnstert.2024.12.031. Epub 2025 Jan 3.

DOI:10.1016/j.fertnstert.2024.12.031

PMID:39755138

Abstract

OBJECTIVE

To study the timing of the effect of linzagolix, an oral gonadotropin-releasing hormone receptor antagonist, on significant reduction in heavy menstrual bleeding (HMB) in women with uterine fibroids.

DESIGN

The study used pooled data from PRIMROSE 1 and PRIMROSE 2, two double-blind, similar placebo-controlled trials of linzagolix in the United States and Europe, respectively. Eligible participants were randomized equally across four treatment arms (linzagolix 100 mg and 200 mg, with and without concomitant hormonal add-back therapy [ABT] consisting of 1-mg estradiol and 0.5-mg norethisterone acetate) and one placebo arm. The cumulative incidence of achieving clinically significant HMB reduction and maintaining it to week 24 was compared between the linzagolix arms and the placebo arm using the Kaplan-Meier plots adjusted for confounding by race and study (PRIMROSE 1 vs. PRIMROSE 2).

SUBJECTS

The PRIMROSE trials randomized 1,012 women aged ≥18 years with ultrasound-confirmed uterine fibroids and HMB.

INTERVENTION

Linzagolix (100 mg and 200 mg, with and without hormonal ABT) vs. placebo.

MAIN OUTCOME MEASURES

The main outcome of this analysis was the time to achievement of clinically significant HMB reduction and its maintenance up to week 24.

RESULTS

The onset of action in achieving and maintaining clinically significant HMB reduction was significantly more rapid for the linzagolix treatment arms than for the placebo arm, with a median time of <4 weeks for most linzagolix doses (except 100 mg alone). The fastest onset was seen with linzagolix 200 mg with or without ABT doses, with a median time of only 3 days. The cumulative incidence of achieving clinically significant HMB reduction by week 4 and maintaining it to week 24 was also significantly higher for the linzagolix treatment arms than for the placebo arm. Specifically, across four linzagolix treatment arms, 23.2%-68.1% achieved clinically significant HMB reduction by week 4 and maintained it to week 24 vs. 7.8% for the placebo arm.

CONCLUSION

Linzagolix was associated with a quick effect on reducing clinically significant HMB compared with placebo. Linzagolix, thus, offers a novel noninvasive treatment approach for the rapid management of HMB symptoms in patients with uterine fibroids.

摘要

目的

研究口服促性腺激素释放激素受体拮抗剂林扎戈利克对子宫肌瘤女性月经过多（HMB）显著减少的起效时间。

设计

该研究使用了PRIMROSE 1和PRIMROSE 2的汇总数据，这两项分别在美国和欧洲进行的双盲、类似安慰剂对照的林扎戈利克试验。符合条件的参与者被随机均分为四个治疗组（林扎戈利克100毫克和200毫克，分别联合或不联合由1毫克雌二醇和0.5毫克醋酸炔诺酮组成的激素补充疗法[ABT]）和一个安慰剂组。使用针对种族和研究（PRIMROSE 1与PRIMROSE 2）进行混杂因素调整的Kaplan-Meier图，比较林扎戈利克组和安慰剂组实现临床显著HMB减少并维持至第24周的累积发生率。

研究对象

PRIMROSE试验将1012名年龄≥18岁、经超声确诊患有子宫肌瘤和HMB的女性随机分组。

干预措施

林扎戈利克（100毫克和200毫克，联合或不联合激素ABT）与安慰剂。

主要观察指标

该分析的主要观察指标是实现临床显著HMB减少并维持至第24周的时间。

结果

与安慰剂组相比，林扎戈利克治疗组在实现和维持临床显著HMB减少方面的起效明显更快，大多数林扎戈利克剂量（单独使用100毫克除外）的中位时间<4周。林扎戈利克200毫克联合或不联合ABT剂量的起效最快，中位时间仅为3天。林扎戈利克治疗组在第4周实现临床显著HMB减少并维持至第24周的累积发生率也显著高于安慰剂组。具体而言，在四个林扎戈利克治疗组中，23.2%-68.1%的患者在第4周实现了临床显著HMB减少并维持至第24周，而安慰剂组为7.8%。