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基于基因共表达网络的方法预测不同亚型乳腺癌的预后 miRNA 生物标志物。

Gene co-expression network approach for predicting prognostic microRNA biomarkers in different subtypes of breast cancer.

机构信息

Modeling in Health Research Center, Institute for Futures Studies in Health, Kerman University of Medical Sciences, Kerman, Iran.

Department of Computer Engineering, Gowgan Educational Center, Tabriz Branch, Islamic Azad University, Tabriz, Iran.

出版信息

Genomics. 2020 Jan;112(1):135-143. doi: 10.1016/j.ygeno.2019.01.010. Epub 2019 Feb 5.

DOI:10.1016/j.ygeno.2019.01.010
PMID:30735795
Abstract

New diagnostic miRNA biomarkers for different types of cancer have been studied extensively, particularly for breast cancer (BC), which is a leading cause of death among women and has many different subtypes. In the present study, a systems biology approach was used to find remarkable and novel miRNA biomarkers for five molecular subtypes of BC: luminal A, luminal B, ERBB2, basal-like and normal-like. The mRNA expression data from the five BC subtypes was used to reconstruct co-expression networks. The important mRNA-miRNA interactions were considered when reconstructing the bipartite networks from which the five bipartite sub-networks were reconstructed for further analysis. The novel biomarkers detected for each subtype are as follows: miRNAs 26b-5p and 124-3p for basal-like, 26b-5p, 124-3p and 5011-5p for ERBB2, 26b-5p and 5011-5p for LumA, 124-3p, 26b-5p and 7-5p for LumB and 26b-5p, 124-3p and 193b-3p for normal-like. The roles of the identified miRNAs in the occurrence or development of each subtype of BC remain unclear and should be investigated in future studies. In addition, the target genes of these miRNAs may be critical to the mechanisms underlying each subtype and should be analyzed as therapeutic targets in future studies.

摘要

已经广泛研究了用于不同类型癌症的新型诊断 miRNA 生物标志物,特别是对于乳腺癌 (BC),它是女性死亡的主要原因,并且有许多不同的亚型。在本研究中,采用系统生物学方法寻找五种乳腺癌分子亚型( luminal A 、 luminal B 、 ERBB2 、基底样和正常样)的显著新型 miRNA 生物标志物。使用五种 BC 亚型的 mRNA 表达数据来重建共表达网络。在从其中重建五个二分子网以进行进一步分析的二分网络中,考虑了重要的 mRNA-miRNA 相互作用。为每种亚型检测到的新型生物标志物如下:基底样的 miR-26b-5p 和 miR-124-3p 、 ERBB2 的 miR-26b-5p 、 miR-124-3p 和 miR-5011-5p 、 LumA 的 miR-26b-5p 和 miR-5011-5p 、 LumB 的 miR-124-3p 、 miR-26b-5p 和 miR-7-5p 以及正常样的 miR-26b-5p 、 miR-124-3p 和 miR-193b-3p 。这些 miRNA 在每种 BC 亚型发生或发展中的作用尚不清楚,应该在未来的研究中进行研究。此外,这些 miRNA 的靶基因可能对每种亚型的机制至关重要,应该在未来的研究中作为治疗靶点进行分析。

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