Investigating ticagrelor in a preclinical pipeline as a novel therapeutic to prevent preterm birth.

IF 3.7 3区生物学 Q1 DEVELOPMENTAL BIOLOGY

Reproduction Pub Date : 2024-02-02 Print Date: 2024-03-01 DOI:10.1530/REP-23-0404

Bridget M Arman, Natalie K Binder, Natasha de Alwis, Sally Beard, Anjali Garg, Tu'uhevaha J Kaitu'u-Lino, Natalie J Hannan

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引用次数: 0

Abstract

In brief: Preterm birth is the leading cause of perinatal morbidity and mortality, and new therapies that delay preterm birth and improve neonatal outcomes are urgently needed. This study investigates whether ticagrelor inhibits uterine contractility and inflammation in preclinical in vitro, ex vivo (human) and in vivo (mouse) studies, to explore the potential of repurposing ticagrelor for the prevention of preterm birth.

Abstract: Preterm birth remains a significant global health challenge, affecting approximately 10% of pregnancies and resulting in one million deaths globally every year. Tocolytic agents, used to manage preterm labour, have considerable limitations including lack of efficacy, and adverse side effects, emphasising the urgent need for innovative solutions. Here, we explore repurposing an antiplatelet cardioprotective drug, ticagrelor, as a potential treatment to prevent preterm birth. Ticagrelor has demonstrated pleiotropic actions beyond platelet inhibition, including relaxant effects on smooth muscle cells and anti-inflammatory effects in models of diabetes and sepsis. As preterm birth is underscored by inflammatory processes triggering uterine contractions, these actions position ticagrelor as an attractive candidate for prevention or delay of preterm birth. Utilising primary human myometrial tissue, human myometrial cells, and a mouse model of preterm birth, we investigated ticagrelor's potential as a safe and effective therapy for preterm birth. We showed that ticagrelor did not reduce the frequency or strength of spontaneous muscle contractions of ex vivo myometrial tissue nor did it reduce in vitro inflammation-induced contractility in myometrial cells. Additionally, ticagrelor did not exhibit the anticipated anti-inflammatory effects in myometrial cell culture experiments. In our mouse model of preterm birth, ticagrelor neither improved the preterm birth rate or fetal survival outcomes. Gene expression of pro-inflammatory cytokines and contraction-associated proteins in postpartum mouse uteri were unaltered by ticagrelor. In conclusion, ticagrelor is not a strong candidate to continue investigations in clinical trial for the treatment of preterm labour and prevention of preterm birth.

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研究临床前管道中的替卡格雷（ticagrelor）作为预防早产的新型疗法。

早产仍然是全球健康面临的一项重大挑战，每年约有 10% 的孕妇受到影响，导致全球一百万人死亡。用于控制早产的催产剂有很大的局限性，包括缺乏疗效和不良副作用，因此迫切需要创新的解决方案。在此，我们探讨了将抗血小板心脏保护药物替卡格雷重新用作预防早产的潜在治疗方法。除抑制血小板外，替卡格雷还具有多种效应，包括对平滑肌细胞的松弛作用以及在糖尿病和败血症模型中的抗炎作用。由于早产是由引发子宫收缩的炎症过程引起的，这些作用使替卡格雷成为预防或推迟早产的有吸引力的候选药物。我们利用原始人类子宫肌组织、人类子宫肌细胞和早产小鼠模型，研究了替卡格雷作为一种安全有效的早产疗法的潜力。我们发现，替卡格雷不会降低体外子宫肌组织自发肌肉收缩的频率或强度，也不会降低体外炎症诱导的子宫肌细胞收缩力。此外，在子宫肌细胞培养实验中，替卡格雷也没有表现出预期的抗炎效果。在我们的早产小鼠模型中，替卡格雷既没有改善早产率，也没有改善胎儿存活率。产后小鼠子宫中促炎细胞因子和子宫收缩相关蛋白的基因表达没有受到替卡格雷的影响。总之，在治疗早产和预防早产的临床试验中，ticagrelor并不是一个强有力的候选药物。

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

Reproduction 生物-发育生物学

CiteScore

7.40

自引率

2.60%

发文量

199

审稿时长

4-8 weeks

期刊介绍： Reproduction is the official journal of the Society of Reproduction and Fertility (SRF). It was formed in 2001 when the Society merged its two journals, the Journal of Reproduction and Fertility and Reviews of Reproduction. Reproduction publishes original research articles and topical reviews on the subject of reproductive and developmental biology, and reproductive medicine. The journal will consider publication of high-quality meta-analyses; these should be submitted to the research papers category. The journal considers studies in humans and all animal species, and will publish clinical studies if they advance our understanding of the underlying causes and/or mechanisms of disease. Scientific excellence and broad interest to our readership are the most important criteria during the peer review process. The journal publishes articles that make a clear advance in the field, whether of mechanistic, descriptive or technical focus. Articles that substantiate new or controversial reports are welcomed if they are noteworthy and advance the field. Topics include, but are not limited to, reproductive immunology, reproductive toxicology, stem cells, environmental effects on reproductive potential and health (eg obesity), extracellular vesicles, fertility preservation and epigenetic effects on reproductive and developmental processes.