Genetic alteration of mRNA editing enzyme APOBEC3B in the pathogenesis of ovarian endometriosis

IF 3.7 2区 医学 Q1 OBSTETRICS & GYNECOLOGY
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引用次数: 0

Abstract

Research question

What are the specific genetic alterations and associated network in endometriotic cells responsible for the disease pathogenesis?

Design

Case control experimental study involving 45 women with endometriosis who underwent laparoscopic surgery (case) and 45 normal samples from women undergoing total abdominal hysterectomy (control). The endometrial samples were subjected to whole exome sequencing (WES) of endometriotic tissue and copy number variation analysis. Validation of gene hits were obtained from WES using polymerase chain reaction techniques, immunological techniques, in-silico tools and transgenic cell line models.

Results

Germline heterozygous deletion of mRNA editing enzyme subunit APOBEC3B was identified in about 96% of endometriosis samples. The presence of germline deletion was confirmed with blood, endometrium and normal ovary samples obtained from the same patient. APOBEC3B deletions resulted in a hybrid protein that activates A1CF. APOBEC3B deletion can be a major cause of changes in the endometriotic microenvironment, and contributes to the pathogenesis and manifestation of the disease. The effect of APOBEC3B deletion was proved by in-vitro experiments in a cell line model, which displayed endometriosis-like characteristics. APOBEC3B germline deletion plays a major role in the pathogenesis of endometriosis, which is evident by the activation of A1CF, an increase in epithelial to mesenchymal transition, cellular proliferation, inflammation markers and a decrease in apoptosis markers.

Conclusion

The deleterious effects caused by APOBEC3B deletion in endometriosis were identified and confirmed. These results might provide a base for identifying the complete pathogenetic mechanism of endometriosis, thereby moving a step closer to better diagnosis and treatment options.

mRNA编辑酶APOBEC3B在卵巢子宫内膜异位症发病机制中的基因改变
研究问题子宫内膜异位症细胞中导致疾病发病机制的特定基因改变和相关网络是什么?设计病例对照实验研究,涉及 45 名接受腹腔镜手术的子宫内膜异位症妇女(病例)和 45 名接受全腹子宫切除术的正常妇女样本(对照)。对子宫内膜样本进行了子宫内膜异位组织全外显子组测序(WES)和拷贝数变异分析。利用聚合酶链式反应技术、免疫学技术、硅内工具和转基因细胞系模型对 WES 中的基因进行了验证。结果在约 96% 的子宫内膜异位症样本中发现了 mRNA 编辑酶亚基 APOBEC3B 的种系杂合缺失。同一患者的血液、子宫内膜和正常卵巢样本均证实存在种系缺失。APOBEC3B 基因缺失产生的杂交蛋白可激活 A1CF。APOBEC3B 基因缺失可能是子宫内膜异位症微环境变化的主要原因,并有助于该疾病的发病机制和表现。APOBEC3B缺失的影响已通过细胞系模型的体外实验得到证实,该模型显示出子宫内膜异位症样特征。APOBEC3B种系缺失在子宫内膜异位症的发病机制中起着重要作用,这体现在A1CF的激活、上皮到间质转化的增加、细胞增殖、炎症标志物和凋亡标志物的减少等方面。这些结果可能为确定子宫内膜异位症的完整发病机制提供了依据,从而向更好的诊断和治疗方案迈进了一步。
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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.
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