The effect of GnRH-a on the angiogenesis of endometriosis

Theodoros Filindris, Efthymia Papakonstantinou, Maria Keramida, Eleftherios Panteris, Sotiris Kalogeropoulos, Neoklis Georgopoulos, Fuminori Taniguchi, George Adonakis, Tasuku Harada, Apostolos Kaponis
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Abstract

Purpose

Neoangiogenesis is necessary for adhesion and invasiveness of endometriotic lesions in women affected by endometriosis. Vascular endothelial growth factor (VEGF) is one of the main components of angiogenesis and is part of the major pathway tissue factor (TF)-protease activated receptor-2 (PAR-2)-VEGF that leads to neoangiogenesis. Specificity protein 1 (SP1) is a transcriptional factor that has recently been studied for its crucial role in angiogenesis via a specific pathway. We hypothesize that by blocking angiogenetic pathways we can suppress endometriotic lesions. Gonadotrophin-releasing hormone-agonists (GnRH-a) are routinely used, especially preoperatively, in endometriosis. It would be of great interest to clarify which angiogenetic pathways are affected and, thereby, pave the way for further research into antiangiogenetic effects on endometriosis.

Methods

We used quantitative real-time polymerase chain reaction (qRT-PCR) to study mRNA expression levels of TF, PAR-2, VEGF, and SP1 in endometriotic tissues of women who underwent surgery for endometriosis and received GnRH-a (leuprolide acetate) preoperatively.

Results

VEGF, TF, and PAR-2 expression is significantly lower in patients who received treatment (p < 0,001) compared to those who did not, whereas SP1 expression is not altered (p = 0.779).

Conclusions

GnRH-a administration does affect some pathways of angiogenesis in endometriotic lesions, but not all of them. Therefore, supplementary treatments that affect the SP1 pathway of angiogenesis should be developed to enhance the antiangiogenetic effect of GnRH-a in patients with endometriosis.

Trial registration

Clinicaltrial.gov ID: NCT06106932.

Abstract Image

GnRH-a 对子宫内膜异位症血管生成的影响
目的 新血管生成是受子宫内膜异位症影响的妇女子宫内膜异位症病灶粘连和侵袭性的必要条件。血管内皮生长因子(VEGF)是血管生成的主要成分之一,也是导致新血管生成的主要途径组织因子(TF)-保护酶激活受体-2(PAR-2)-VEGF的一部分。特异性蛋白 1(SP1)是一种转录因子,最近研究发现它在通过特异性途径促进血管生成方面发挥着关键作用。我们假设,通过阻断血管生成途径,可以抑制子宫内膜异位症病变。促性腺激素释放激素激动剂(GnRH-a)是子宫内膜异位症的常规用药,尤其是术前用药。我们使用定量实时聚合酶链反应(qRT-PCR)研究了因子宫内膜异位症接受手术并在术前接受 GnRH-a(醋酸亮丙瑞林)治疗的女性子宫内膜异位症组织中 TF、PAR-2、VEGF 和 SP1 的 mRNA 表达水平。结果与未接受治疗的患者相比,接受治疗的患者血管内皮生长因子、TF 和 PAR-2 的表达明显降低(p < 0,001),而 SP1 的表达没有改变(p = 0.779)。因此,应开发影响血管生成的 SP1 通路的辅助治疗方法,以增强 GnRH-a 对子宫内膜异位症患者的抗血管生成作用:NCT06106932。
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