患者反复种植失败和不孕与子宫内膜拷贝数变异导致的整合素 B3 升高密切相关。

IF 2.8 Q2 REPRODUCTIVE BIOLOGY
Hong-Xia Xu, Sheng-Ni Liu, Xiaoyi Xiang, Yan Lei, Yun-Xiu Li, Xiang-Jing Tang, Jian-Mei Yu, Li-Mei Tao, Ze Wu, Li Li
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引用次数: 0

摘要

本研究揭示了基因拷贝数变异(CNVs)与子宫内膜组织整合素表达之间的关系,特别是关注反复植入失败和不明原因不孕的患者。通过对48例重复着床失败患者和10例无着床史的不孕症患者子宫内膜标本进行分析,研究CNV表达、整合素αVβ3(实时定量聚合酶链反应和蛋白免疫印迹法)及相关临床指标。结果显示,约31.04%的不孕症患者存在CNV,主要影响染色体2、5、6、7、10、11、15、19和x。年龄与CNV的发生有关。在重复植入失败患者中,整合素β3在CNV组的表达明显高于非CNV组。与凝血相关的临床指标在CNV组和非CNV组之间存在显著差异。该研究表明,CNVs、整合素β3表达增加和反复植入失败之间存在潜在关联。该研究通过整合先进的分子诊断技术,为理解遗传变异、整合素功能和凝血因子之间复杂的相互作用提供了新的信息,从而强调了生殖医学个性化方法的必要性。这些结果可能重新定义复发性植入失败的诊断范式,为未来的转化应用奠定基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Repeated implantation failures and infertility in patients are strongly associated with elevated integrin B3 due to endometrial copy number variation.

This study reveals the association between gene copy number variants (CNVs) and integrin expression in endometrial tissue, especially focusing on patients with repeated implantation failure and unexplained infertility. The CNV expression, integrin αVβ3 (by real-time quantitative polymerase chain reaction and protein immunoblotting), and related clinical indicators were investigated by analyzing endometrial samples from 48 patients with repeated implantation failures and 10 patients with infertility and with no history of implantation issues. The results revealed the presence of CNVs in approximately 31.04% of patients with infertility, mainly affecting chromosomes 2, 5, 6, 7, 10, 11, 15, 19, and X. Age was associated with CNV occurrence. Integrin β3 expression was significantly higher in the CNV group than in the non-CNV group among patients with repeated implant failure. Clinical indicators related to coagulation were significantly different between the CNV and non-CNV groups. The study indicated a potential association between CNVs, increased integrin β3 expression, and recurrent implant failure. The study provides new information for understanding the complex interactions between genetic variants, integrin function, and coagulation factors by integrating advanced molecular diagnostic techniques, thereby emphasizing the need for a personalized approach in reproductive medicine. These results may redefine the diagnostic paradigm for recurrent implantation failure, laying the foundation for future translational applications.

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