Uterine fibroids: a look at the problem

R. A. Karamyan, I. M. Ordiyats, V. Khorolskiy, D. R. Asatryan
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Abstract

Despite scientific progress, there is currently no sigle opinion about the cause of the occurrence and recurrence of uterine fibroids, but due to the high level of molecular medicine, progress is being made in the hormonal and molecular genetic mechanisms of initiation, formation and growth of the fibroisds. The issue of pathogenetic treatment and prevention of recurrence of uterine fibroids in reproductive age remains relevant. The aims of the review. The aim of this review is to summarize current data about microRNA in biology of uterine leiomyoma (LM). This information can improve our understanding of the broad molecular interaction of signaling pathways in the formation of LM, and further maintaining epigenetic regulation as an important mechanism in the pathogenesis of uterine leiomyoma. In leiomyomas, the expression of a number of non-proteincoding genes is altered, such as microRNAs (miRNAs), which target genes that code protein. Material and research methods. Original and review articles, book chapters in the PubMed database related to the study of the pathogenesis of uterine fibroids in the period from 2004 to 2022 were found and analyzed. Results and discussions. Based on an analytical review of the literature, it becomes obvious that as evidence should be considered: 1. Abnormal myometrial and fibroid stem cells show an increased response to estrogen and progesterone exposure, stimulating processes such as cell proliferation, inhibition of apoptosis, and extracellular matrix (ECM) formation. 2. A number of tumor suppressor genes are abnormally hypermethylated in the LM when compared to normal myometrium, genes that form and regulate collagen, and a subset of estrogen receptor genes. 3. Multiple studies using microarray analysis or sequencing have demonstrated the existence of dysregulation of a number of protein-coding genes involved in cell proliferation and apoptosis, which are critical for the growth and progression of uterine fibroids. There are no reliable evidence base and do not provide an opportunity for practical application of clinically significant risk factors, the possibility of mathematical prediction of the growth of uterine fibroids in women of reproductive age. Data on the effect of the expression of a number of microRNAs on the growth of uterine fibroids in vivo are rather contradictory. The epigenetic processes of regulation and pathogenesis of the growth of leiofibromyomas in reproductive age have not been fully studied and substantiated. There are practically no data on predicting the growth of uterine fibroids in reproductive age, which will allow us to assess the risk of growth and determine further treatment tactics. Conclusion. Further work on the identification of specific genes, miRNAs, that are involved in the pathogenesis of LM may inspire the creation of new pathogenetic treatments. Such treatment is especially relevant for those groups of patients of reproductive age for whom surgical treatment may be ineffective. Targeted treatment can also prevent the recurrence of uterine fibroids, hence the need for repeat surgery.
子宫肌瘤:一看问题
尽管科学进步了,但目前对于子宫肌瘤发生和复发的原因还没有统一的看法,但由于分子医学的高水平,对子宫肌瘤发生、形成和生长的激素和分子遗传机制的研究正在取得进展。对育龄期子宫肌瘤的发病、治疗和预防仍有重要意义。审查的目的。本文就microRNA在子宫平滑肌瘤(LM)生物学中的研究进展进行综述。这些信息有助于我们进一步了解LM形成过程中信号通路的广泛分子相互作用,并进一步维持表观遗传调控在子宫平滑肌瘤发病中的重要机制。在平滑肌瘤中,一些非蛋白编码基因的表达发生了改变,例如靶向编码蛋白基因的microRNAs (miRNAs)。材料和研究方法。对PubMed数据库中2004年至2022年期间有关子宫肌瘤发病机制研究的原创文章、综述文章、书籍章节进行分析。结果和讨论。基于对文献的分析回顾,很明显,作为证据应该考虑:1。异常子宫肌瘤和肌瘤干细胞对雌激素和黄体酮暴露的反应增加,刺激细胞增殖、抑制细胞凋亡和细胞外基质(ECM)形成等过程。2. 与正常肌层、形成和调节胶原蛋白的基因以及雌激素受体基因亚群相比,LM中许多肿瘤抑制基因异常高甲基化。3.利用微阵列分析或测序的多项研究表明,一些参与细胞增殖和凋亡的蛋白质编码基因存在失调,这些基因对子宫肌瘤的生长和进展至关重要。目前尚无可靠的证据基础,也没有为实际应用提供机会,对临床显著的危险因素进行数学预测育龄妇女子宫肌瘤生长的可能性。一些microrna的表达在体内对子宫肌瘤生长的影响的数据比较矛盾。育龄期子宫肌瘤生长的调控和发病机制的表观遗传过程尚未得到充分的研究和证实。几乎没有数据预测子宫肌瘤在育龄期的生长,这将使我们能够评估其生长的风险并确定进一步的治疗策略。结论。进一步鉴定LM发病机制中涉及的特定基因,mirna,可能会激发新的发病治疗方法的创造。这种治疗对于那些手术治疗可能无效的育龄患者群体尤其重要。有针对性的治疗也可以防止子宫肌瘤的复发,因此需要重复手术。
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