RB1和miR-132在乳腺导管癌中的下调

Mohammad Abbasi-Kolli, Shirin Shahbazi, Loabat Geranpayeh
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摘要

引言:miR-132-3p在正常乳腺发育中起作用,其下调在乳腺癌中已被证实。miR-132-3p的靶标之一是RB1,它在乳腺癌中也失活。RB1和miR-132之间的相互作用已经在几种病理条件下被报道。我们的目的是研究miR-132和RB1在乳腺导管癌中的表达水平之间的相关性。方法:对女性原发性乳腺癌患者的组织进行研究。根据临床和病理资料对肿瘤标本进行分类。通过RNA提取和cDNA合成,比较肿瘤组织与癌旁组织的相关基因表达。通过相关系数检验评估RB1与miR-132之间的联系。结果:我们的研究结果显示miR-132和RB1表达显著降低,比值分别为0.165和0.365。肿瘤分级与miRNA-132水平相关。miR-132在I级肿瘤中的表达与正常邻近组织基本相等,但在II级和III级肿瘤中表达强烈降低。相关分析显示RB1与miR-132水平之间存在较小的线性关联。结论:miR-132和RB1表达的降低证实了这两个基因在乳腺癌中的肿瘤抑制作用。考虑到RB1是miR-132的靶点之一,需要进一步的研究来发现mirna介导的miR-132的上调作用。我们的发现发现miR-132和RB1之间存在小的线性关联,这可以推断它们在乳腺癌发病机制中的独立功能。
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Down-regulation of RB1 and miR-132 in ductal carcinoma of the breast.

Introduction: miR-132-3p acts in normal breast development and its downregulation has been documented in breast cancer. One of the targets of miR-132-3p is RB1 which is also inactivated in breast cancer. The interactions between RB1 and miR-132 have been reported in several pathological conditions. We aimed to investigate the correlation between expression levels of miR-132 and RB1 in ductal carcinoma of the breast.

Methods: The study was carried out on tissues obtained from female patients with primary breast cancer. Tumor samples were classified using clinical and pathological data. Following RNA extraction and cDNA synthesis, relative gene expressions in tumors were compared to non-cancerous adjacent tissues. The link between RB1 and miR-132 was assessed by the correlation coefficient test.

Results: Our findings revealed a significant decrease in miR-132 and RB1 expressions with a ratio of 0.165 and 0.365, respectively. Tumor grade showed an association with miRNA-132 levels. The expression of miR-132 in grade I tumors was almost equal to that of normal adjacent tissues, but was intensely decreased in grades II and III. The correlation analysis showed a small linear association between RB1 and miR-132 levels.

Conclusion: The reduction of miR-132 and RB1 expression confirmed the tumor-suppressive role of both genes in breast cancer. Considering that RB1 is one of the miR-132 targets, further studies are required to discover any miRNA-mediated upregulation role for miR-132. Our finding discovered a small linear association between miR-132 and RB1, which can be concluded towards their independent function in breast cancer pathogenesis.

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