单细胞 RNA 测序揭示了卵巢早衰患者卵泡免疫细胞和颗粒细胞之间的共同相互作用。

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-11-08 DOI:10.1093/biolre/ioae157
Ying Han, Junrong Diao, Xinyan Wang, Shuai Zhang, Lina Yuan, Yaqiong Ping, Ge Gao, Yunshan Zhang, Haining Luo
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引用次数: 0

摘要

目的研究卵巢早衰(POI)、卵巢储备功能正常(Normal)和高龄产妇(AMA)的卵泡微环境,并确定潜在的治疗靶点:本研究共纳入了9名接受体外受精或卵胞浆内单精子注射的女性,其中包括3名早衰性卵巢功能不全女性、3名正常女性和3名高龄产妇。对每位受试者的第一个不含积层细胞的穿刺卵泡进行单细胞RNA测序,以探讨POI、正常和AMA受试者卵泡微环境的特征:共分离出 87323 个细胞,并将其分为六组:结果:共分离出 87323 个细胞,并将其分为六组:T 细胞、B 细胞、中性粒细胞、嗜碱性粒细胞、单核吞噬细胞和颗粒细胞。进一步的分析表明,在 AMA 和 POI 患者中,第 6 组颗粒细胞的数量增加,而γ δ T 细胞(GDT)的数量减少。我们还发现,GDT 细胞和单核细胞之间差异表达的基因富集于核糖体和内质网(ER)相关通路。此外,研究还表明,与正常组相比,AMA 和 POI 患者单核细胞与颗粒细胞之间的 VEGFA-FLT1 相互作用可能消失:结论:单核细胞和颗粒细胞中 VEGFA-FLT1 相互作用的丧失,以及 ER 和核糖体相关通路的丰富,可能会驱动过度炎症,加速颗粒细胞衰老并导致不孕。这项研究为 POI 和衰老的发病机制提供了新的见解,并强调了 VEGFA/FLT1 相互作用可能是减少炎症和治疗 POI 的潜在治疗靶点。
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Single-cell RNA sequencing reveals common interactions between follicle immune cells and granulosa cells in premature ovarian insufficiency patients.

Objective: To investigate the follicle microenvironment of individuals with premature ovarian insufficiency (POI), normal ovarian reserve (normal) and advanced maternal age (AMA), and identify potential therapeutic targets.

Methods: A total of 9 women, including 3 POI, 3 normal and 3 AMA women, underwent in vitro fertilization or intracytoplasmic sperm injection were included in this study. For each participant, the first punctured follicle not containing cumulus cells were submitted to single-cell RNA sequencing to explore the characteristics of the follicle microenvironment of POI, normal and AMA individuals.

Result(s): A total of 87,323 cells were isolated and grouped into six clusters: T cells, B cells, neutrophils, basophils, mononuclear phagocytes, and granulosa cells. Further analysis demonstrated that the population of granulosa cells in cluster 6 was increased in AMA and POI patients, whereas the population of gamma delta T (GDT)-cells was decreased. We also found that the genes that were differentially expressed between GDT cells and monocytes were enriched in ribosome- and endoplasmic reticulum (ER)-related pathways. In addition, it showed that VEGFA-FLT1 interaction between the monocytes and granulosa cells may be lost in the AMA and POI patients as compared with the normal group.

Conclusion(s): Loss of the VEGFA-FLT1 interaction in monocytes and granulosa cells, along with enriched ER- and ribosome-related pathways, may drive excess inflammation, accelerating granulosa cell senility and contributing to infertility. This study provides new insights into the pathogenesis of POI and aging and highlights the VEGFA/FLT1 interaction may be a potential therapeutic target for reducing inflammation and treating POI.

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4.30%
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567
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