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子宫肌瘤中的孕酮信号传导:分子机制与治疗机遇

Progesterone signaling in uterine fibroids: Molecular mechanisms and therapeutic opportunities.

作者信息

Ploumaki Ioanna, Macri Valeria I, Segars James H, Islam Md Soriful

机构信息

School of Medicine at National and Kapodistrian University of Athens, Athens 157 72, Greece.

Department of Gynecology and Obstetrics, Division of Reproductive Sciences & Women's Health Research, Johns Hopkins Medicine, Baltimore, MD 21205, USA.

出版信息

Life Sci. 2025 Feb 1;362:123345. doi: 10.1016/j.lfs.2024.123345. Epub 2024 Dec 29.

Abstract

Progesterone (P4) is a vital female sex hormone involved in various physiological processes, including the maintenance of the endometrium, mammary gland development, and bone health. Beyond its reproductive roles, P4 is implicated in the pathogenesis of hormone-dependent conditions like uterine fibroids, the most common benign tumors in women, which can severely affect quality of life and fertility. Traditionally, estrogen was considered the primary driver of fibroid growth, but recent research highlights the significant role of P4 in fibroid growth. P4 interacts with progesterone receptors (PRs) and non-genomic membrane receptors (mPRs and PGRMCs) to activate signaling pathways that enhance tumor growth and survival. P4 promotes vascular changes that improve the blood supply to fibroids and modifies the extracellular matrix, a key component of fibroid structure. This understanding has led to the investigation of selective progesterone receptor modulators (SPRMs) as potential therapies for fibroids. Clinical trials have demonstrated the effectiveness of SPRMs like mifepristone, asoprisnil, and ulipristal acetate in reducing fibroid size and symptoms, though concerns about safety, particularly with long-term use, remain. Newer SPRMs, such as vilaprisan, show promise, but further research is necessary to assess the long-term safety and effectiveness. This review discusses the mechanisms by which progesterone contributes to fibroid growth and examines clinical effectiveness of SPRMs as potential treatments for uterine fibroids.

摘要

孕酮(P4)是一种重要的女性性激素,参与多种生理过程,包括子宫内膜的维持、乳腺发育和骨骼健康。除了其生殖作用外,P4还与激素依赖性疾病如子宫肌瘤的发病机制有关,子宫肌瘤是女性最常见的良性肿瘤,可严重影响生活质量和生育能力。传统上,雌激素被认为是肌瘤生长的主要驱动因素,但最近的研究突出了P4在肌瘤生长中的重要作用。P4与孕酮受体(PRs)以及非基因组膜受体(mPRs和PGRMCs)相互作用,激活增强肿瘤生长和存活的信号通路。P4促进血管变化,改善肌瘤的血液供应,并改变细胞外基质,而细胞外基质是肌瘤结构的关键组成部分。这种认识促使人们研究选择性孕酮受体调节剂(SPRMs)作为肌瘤的潜在治疗方法。临床试验已经证明米非司酮、阿索普尼尔和醋酸乌利司他等SPRMs在缩小肌瘤大小和缓解症状方面的有效性,不过对安全性的担忧依然存在,尤其是长期使用时。新型SPRMs,如维拉普瑞森,显示出前景,但需要进一步研究来评估其长期安全性和有效性。本综述讨论了孕酮促进肌瘤生长的机制,并探讨了SPRMs作为子宫肌瘤潜在治疗方法的临床有效性。

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