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微小RNA基因甲基化水平与乳腺癌表达水平及病理形态学特征的关系

Relationship of the Levels of microRNA Gene Methylation with the Level of Their Expression and Pathomorphological Characteristics of Breast Cancer.

作者信息

Filippova E A, Pronina I V, Lukina S S, Kazubskaya T P, Braga E A, Burdennyi A M, Loginov V I

机构信息

Research Institute of General Pathology and Pathophysiology, Moscow, Russia.

N. N. Blokhin National Medical Research Center of Oncology, Ministry of Health of the Russian Federation, Moscow, Russia.

出版信息

Bull Exp Biol Med. 2021 Oct;171(6):764-769. doi: 10.1007/s10517-021-05312-2. Epub 2021 Oct 27.

Abstract

We studied the relationship of the levels of microRNA group expression and methylation with clinical and pathomorphological parameters of breast cancer and its immunohistochemical status. Quantitative methylation specific PCR analysis showed a significant (p<0.001) increase in the methylation level of 4 microRNA genes (MIR127, MIR129-2, MIR132, and MIR148A) and a significant (p<0.001) decrease for gene MIR375 relative to paired histologically normal tissue. Real-time PCR analysis revealed a significant (p≤0.001) decrease in the expression of 4 microRNAs (miR-127-5p, miR-129-5p, miR-132-3p, and miR-148a-3p) and a significant (p≤0.001) increase in the expression of miR-375-3p. A significant (rs=-0.6--0.7, p≤0.001) relationship between changes in the expression level of miR-129-5p, miR-132-3p, miR-148a-3p, and miR-375-3p and the levels of methylation of the corresponding genes in breast cancer was showed by using Spearman's rank correlation test. Analysis of the samples with consideration of the pathophysiological characteristics of the tumor revealed two significant markers of tumor progression: MIR129-2/miR-129-5p and MIR375/miR-375-3p. Both factors, the increase in the level of MIR129-2 methylation (p<0.001) and a decrease in the expression level of miR-129-5p (p<0.001), are significantly associated (p<0.001) with stage III/IV and the absence of HER2 expression. For MIR375/miR-375-3p, on the contrary, an association of low methylation level and enhanced expression with increased Ki-67 level (>30%, p<0.05) was revealed. These findings are of interest for understanding the mechanisms of breast cancer development and can provide the basis for the diagnosis and prognosis of the course of this disease. Moreover, the revealed features can be useful for adjusting the course of treatment with consideration of the pathophysiological characteristics of the tumor.

摘要

我们研究了微小RNA组表达水平和甲基化与乳腺癌临床及病理形态学参数及其免疫组化状态之间的关系。定量甲基化特异性PCR分析显示,相对于配对的组织学正常组织,4个微小RNA基因(MIR127、MIR129 - 2、MIR132和MIR148A)的甲基化水平显著升高(p<0.001),而基因MIR375的甲基化水平显著降低(p<0.001)。实时PCR分析显示,4种微小RNA(miR - 127 - 5p、miR - 129 - 5p、miR - 132 - 3p和miR - 148a - 3p)的表达显著降低(p≤0.001),而miR - 375 - 3p的表达显著升高(p≤0.001)。使用Spearman等级相关检验显示,miR - 129 - 5p、miR - 132 - 3p、miR - 148a - 3p和miR - 375 - 3p表达水平的变化与乳腺癌中相应基因的甲基化水平之间存在显著相关性(rs = - 0.6 - - 0.7,p≤0.001)。考虑肿瘤病理生理特征对样本进行分析,发现了两个肿瘤进展的显著标志物:MIR129 - 2/miR - 129 - 5p和MIR375/miR - 375 - 3p。MIR129 - 2甲基化水平升高(p<0.001)和miR - 129 - 5p表达水平降低(p<0.001)这两个因素均与III/IV期及HER2表达缺失显著相关(p<0.001)。相反,对于MIR375/miR - 375 - 3p,发现低甲基化水平和增强表达与Ki - 67水平升高(>30%,p<0.05)相关。这些发现对于理解乳腺癌的发生机制具有重要意义,可为该疾病病程的诊断和预后提供依据。此外,所揭示的特征对于根据肿瘤病理生理特征调整治疗方案可能有用。

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