Receptive window might be shorter in patients with endometriosis and lesions cyclically prepare for implantation

F&S science Pub Date : 2025-05-01 DOI:10.1016/j.xfss.2024.11.002

Nirukshi Samarajeewa Ph.D. , Sophea Heng Ph.D. , Ying Li B.Eng. , Maxine Scelwyn M.D. , Luk J. Rombauts M.D. Ph.D. , Guiying Nie Ph.D.

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Abstract

Objective

To investigate whether endometrial receptivity is affected in patients with endometriosis using podocalyxin (PCX) as a functional biomarker and to study how endometriotic lesions display PCX and the potential pathological implications.

Design

We have previously reported that PCX, an anti-adhesion glycoprotein and barrier protector, is dynamically regulated in the endometrium and acts as a key negative regulator of epithelial receptivity. Early in the cycle both luminal epithelium (LE, lining the endometrial surface) and glandular epithelium (GE, residing within the tissue) strongly express PCX, but in the receptive window, PCX is selectively downregulated in LE, switching the endometrial surface to an adhesive state for embryo attachment/implantation; meanwhile, PCX expression is maintained in GE until postreceptivity. Here, we immuno-stained PCX in endometrial tissues and ectopic lesions biopsied across the menstrual cycle from patients with endometriosis (EOS, n = 41), and compared with endometrium of non-endometriosis controls (non-EOS, n = 55). We further investigated how PCX changes observed in ectopic lesions may influence their adhesive capacity.

Subjects

Women without and with endometriosis.

Exposure

Not applicable.

Main Outcome Measures

The window of endometrial receptivity might be shorter in patients with endometriosis; ectopic sites in addition downregulate PCX cyclically, mirroring the eutopic endometrial cells in preparing for receptivity to increase their adhesion potential.

Results

Endometrial PCX levels were comparable between non-EOS and EOS early in the cycle, and in both groups, PCX is downregulated in LE during the expected window of receptivity; however, in EOS endometrium, PCX is reduced earlier in GE as if the receptive window were shorter. In endometriotic lesions, PCX was detected in endometrial LE- and GE-like cells plus mesothelial cells enveloping peritoneal organs, but PCX was cyclically lost specifically in LE-like cells and reduced in GE-like cells as seen in the eutopic endometrium, which however may increase their adhesion potential to nearby organs (overlaid by mesothelial cells). This speculation was further corroborated in an in vitro model showing endometrial epithelial cells with lower PCX were indeed more adhesive to mesothelial cells.

Conclusion

Endometrial receptivity is subtly affected in patients with endometriosis with a shorter window. Cyclic downregulation of PCX in ectopic sites may have pathological consequences.

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子宫内膜异位症患者的接受窗口可能较短，病变周期准备着床。

目的：探讨子宫内膜异位症患者子宫内膜容受性是否受足alyxin （PCX）功能标志物的影响；研究子宫内膜异位病变如何显示PCX及其潜在的病理意义。设计：我们之前报道过PCX，一种抗黏附糖蛋白和屏障保护器，在子宫内膜中受到动态调节，并作为上皮接受性的关键负调节因子。在周期早期，子宫内膜上皮（LE，衬在子宫内膜表面）和腺体上皮（GE，位于组织内）都强烈表达PCX，但在接受期窗口，PCX在LE中被选择性下调，将子宫内膜表面转换为胚胎附着/着床的粘附状态；同时，PCX在GE中的表达一直维持到接受后。在这里，我们对子宫内膜异位症患者（n=41）的子宫内膜组织和异位病变进行了免疫染色的PCX，并与非子宫内膜异位症对照组（n=55）的子宫内膜进行了比较。我们进一步研究了在异位病变中观察到的PCX变化如何影响其粘附能力。研究对象：无子宫内膜异位症和有子宫内膜异位症的女性。曝光:N / A。主要观察指标：子宫内膜异位症患者子宫内膜容受性窗口期可能较短；异位部位也周期性下调PCX，反映异位子宫内膜细胞为接受性做准备，以增加其粘附潜力。结果：子宫内膜PCX水平在周期早期在非EOS和EOS之间是相当的，在预期的接受窗口期间，两组的PCX在LE中下调，然而，EOS子宫内膜PCX在GE中较早降低，好像接受窗口较短。在子宫内膜异位症病变中，PCX在子宫内膜LE样细胞和ge样细胞以及包围腹膜器官的间皮细胞中检测到，但PCX在LE样细胞中周期性丢失，在异位子宫内膜ge样细胞中减少，但这可能增加了它们对附近器官的粘附潜力（被间皮细胞覆盖）。这一推测在体外模型中得到进一步证实，显示PCX较低的子宫内膜上皮细胞确实更能粘附间皮细胞。结论：短窗期子宫内膜异位症患者子宫内膜容受性受到微妙影响。异位部位PCX的循环下调可能有病理后果。

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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