利用子宫内膜器官组织解密子宫肌瘤患者的子宫内膜功能障碍:一项试点研究

IF 3.7 2区 医学 Q1 OBSTETRICS & GYNECOLOGY Reproductive biomedicine online Pub Date : 2024-07-03 DOI:10.1016/j.rbmo.2024.104355
Yu Zhang , Minghui Lu , Yanli Han , Boyang Liu , Rusong Zhao , Peishu Liu , Han Zhao
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引用次数: 0

摘要

研究问题子宫内膜肌瘤对子宫内膜有什么影响,这种影响是如何介导的?设计收集了13名患有非腔隙扭曲型子宫内膜肌瘤(直径≤4厘米;国际妇产科联盟4型)的患者和13名因良性宫颈疾病接受子宫切除术的无肌瘤患者的子宫内膜,他们的临床基线相似。子宫内膜器官组织在体外建立,并通过雌激素和孕激素诱导其进入分泌期。对来自三名子宫肌瘤患者和三名对照组患者的未处理期和分泌期子宫内膜有机体进行了转录组测序。结果数据显示,未经治疗的子宫肌瘤患者的子宫内膜器官组织中激素受体(PGR)水平异常升高,可能导致腺体和血管发育异常。对雌激素和孕激素的异常反应促使对分泌期进行进一步研究。有肌瘤的分泌期子宫内膜类器官组织的乙酰基-α-微管蛋白、ODF2 和 TPPP(表明纤毛可能减少)以及 COL6A1(作为细胞外基质(ECM)模型增加的标志物)发生了较大变化。未经处理和患有肌瘤的分泌性子宫内膜有机体都显示出与 ECM 机械传导相关的基因和通路的上调。这项研究首次揭示了壁内肌瘤在未经处理的分泌性子宫内膜有机体中创造了异常的激素和机械环境。壁内肌瘤对与子宫内膜腺体、血管、纤毛和 ECM 相关的基因表达产生了负面影响,表明壁内肌瘤损害了子宫内膜的蜕膜化和接受能力。
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Deciphering endometrial dysfunction in patients with uterine myoma using endometrial organoids: a pilot study

Research question

What influence does an intramural myoma have on the endometrium, and how is this mediated?

Design

Endometrium was collected from 13 patients with non-cavity-distorting intramural myomas (diameter ≤4 cm; International Federation of Gynecology and Obstetrics type 4) and 13 patients without myomas undergoing hysterectomy for benign cervical diseases with a similar clinical baseline. Endometrial organoids were established in vitro and induced to reach the secretory phase by oestrogen and progesterone. Transcriptome sequencing was conducted on endometrial organoids in both untreated and secretory stages from three individuals with myomas and three control participants. Immunofluorescence and real-time quantitative PCR (RT-qPCR) were performed on endometrial organoids from another 10 myoma patients and 10 control patients for validation.

Results

The data revealed abnormally increased hormone receptor (PGR) levels in the untreated endometrial organoids with myomas, resulting in potentially abnormal glandular and vascular development. The aberrant responses to oestrogen and progestogen prompted further investigation into the secretory phase. The secretory endometrial organoids with myomas exhibited greater changes in acetyl-α-tubulin, ODF2 and TPPP, demonstrating likely decreased cilia, and COL6A1, used as a marker for increased extracellular matrix (ECM) modelling. Both untreated and secretory endometrial organoids with myoma showed an up-regulation of genes and pathways related to ECM mechanotransduction. The expression pattern of receptivity-related genes was disturbed in endometrial organoids with myoma.

Conclusions

This study is the first to reveal that intramural myomas create an abnormal hormonal and mechanical environment in the untreated and secretory endometrial organoids. The intramural myomas negatively impacted gene expression relating to endometrial glands, blood vessels, cilia and ECM, indicating that intramural myomas impair endometrial decidualization and receptivity.

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来源期刊
Reproductive biomedicine online
Reproductive biomedicine online 医学-妇产科学
CiteScore
7.20
自引率
7.50%
发文量
391
审稿时长
50 days
期刊介绍: Reproductive BioMedicine Online covers the formation, growth and differentiation of the human embryo. It is intended to bring to public attention new research on biological and clinical research on human reproduction and the human embryo including relevant studies on animals. It is published by a group of scientists and clinicians working in these fields of study. Its audience comprises researchers, clinicians, practitioners, academics and patients. Context: The period of human embryonic growth covered is between the formation of the primordial germ cells in the fetus until mid-pregnancy. High quality research on lower animals is included if it helps to clarify the human situation. Studies progressing to birth and later are published if they have a direct bearing on events in the earlier stages of pregnancy.
期刊最新文献
Ultra-fast vitrification and rapid elution of human oocytes: part I. germinal vesicle model validation. Ultra-fast vitrification and rapid elution of human oocytes: Part II - verification of blastocyst development from mature oocytes. Inside Front Cover - Affiliations and First page of TOC Front Matter - Continued TOC Outside Back Cover - Editorial Board
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