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Circulating miRNAs in Untreated Breast Cancer: An Exploratory Multimodality Morpho-Functional Study

机译:未经治疗的乳腺癌中的循环miRNA:探索性多模态形态功能研究

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摘要

The aim of this study was to identify new disease-related circulating miRNAs with high diagnostic accuracy for breast cancer (BC) and to correlate their deregulation with the morpho-functional characteristics of the tumour, as assessed in vivo by positron emission tomography/magnetic resonance (PET/MR) imaging. A total of 77 untreated female BC patients underwent same-day PET/MR and blood collection, and 78 healthy donors were recruited as negative controls. The expression profile of 84 human miRNAs was screened by using miRNA PCR arrays and validated by real-time PCR. The validated miRNAs were correlated with the quantitative imaging parameters extracted from the primary BC samples. Circulating miR-125b-5p and miR-143-3p were upregulated in BC plasma and able to discriminate BC patients from healthy subjects (miR-125-5p area under the receiver operating characteristic ROC curve (AUC) = 0.85 and miR-143-3p AUC = 0.80). Circulating CA15-3, a soluble form of the transmembrane glycoprotein Mucin 1 (MUC-1) that is upregulated in epithelial cancer cells of different origins, was combined with miR-125b-5p and improved the diagnostic accuracy from 70% (CA15-3 alone) to 89% (CA15-3 plus miR-125b-5p). MiR-143-3p showed a strong and significant correlation with the stage of the disease, apparent diffusion coefficient (ADCmean), reverse efflux volume transfer constant (Kepmean) and maximum standardized uptake value (SUVmax), and it might represent a biomarker of tumour aggressiveness. Similarly, miR-125b-5p was correlated with stage and grade 2 but inversely correlated with the forward volume transfer constant (Ktransmean) and proliferation index (Ki67), suggesting a potential role as a biomarker of a relatively more favourable prognosis. In situ hybridization (ISH) experiments revealed that miR-143-3p was expressed in endothelial tumour cells, miR-125-5p in cancer-associated fibroblasts, and neither in epithelial tumour cells. Our results suggested that miR-125-5p and miR-143-3p are potential biomarkers for the risk stratification of BC, and Kaplan-Maier plots confirmed this hypothesis. In addition, the combined use of miR-125-b-5p and CA15-3 enhanced the diagnostic accuracy up to 89%. This is the first study that correlates circulating miRNAs with in vivo quantified tumour biology through PET/MR biomarkers. This integration elucidates the link between the plasmatic increase in these two potential circulating biomarkers and the biology of untreated BC. In conclusion, while miR-143-3b and miR-125b-5p provide valuable information for prognosis, a combination of miR-125b-5p with the tumour marker CA15-3 improves sensitivity for BC detection, which warrants consideration by further validation studies.
机译:这项研究的目的是鉴定新的疾病相关循环miRNA,对乳腺癌(BC)具有很高的诊断准确度,并将其解除调节与肿瘤的形态功能特征相关联,如通过正电子发射断层扫描/磁共振在体内评估的那样(PET / MR)成像。共有77名未经治疗的女性BC患者在当天接受PET / MR和血液采集,并招募了78名健康供体作为阴性对照。使用miRNA PCR阵列筛选了84个人类miRNA的表达谱,并通过实时PCR进行了验证。验证的miRNA与从原始BC样品中提取的定量成像参数相关。循环血浆miR-125b-5p和miR-143-3p在BC血浆中上调,并且能够将BC患者与健康受试者区分开(在接收器工作特征ROC曲线(AUC)下的miR-125-5p面积= 0.85和miR-143-p 3p AUC = 0.80)。循环CA15-3是一种可溶形式的跨膜糖蛋白粘蛋白1(MUC-1),在不同来源的上皮癌细胞中上调,将其与miR-125b-5p结合使用,将诊断准确性提高了70%(CA15-3到89%(CA15-3加miR-125b-5p)。 MiR-143-3p与疾病的分期,表观扩散系数(ADCmean),反向外排量传递常数(Kepmean)和最大标准化摄取值(SUVmax)密切相关,并且可能代表了肿瘤的生物标志物进取心。同样,miR-125b-5p与2级和2级相关,但与正向体积转移常数(Ktransmean)和增殖指数(Ki67)则呈负相关,表明其可能作为相对较有利的预后的生物标志物。原位杂交(ISH)实验表明,miR-143-3p在内皮肿瘤细胞中表达,miR-125-5p在癌症相关的成纤维细胞中表达,在上皮肿瘤细胞中均不表达。我们的结果表明,miR-125-5p和miR-143-3p是BC风险分层的潜在生物标志物,Kaplan-Maier曲线证实了这一假设。此外,miR-125-b-5p和CA15-3的组合使用可将诊断准确性提高至89%。这是第一项通过PET / MR生物标志物将循环miRNA与体内定量肿瘤生物学相关联的研究。这种整合阐明了这两种潜在循环生物标记物的血浆增加与未经治疗的BC生物学之间的联系。总之,尽管miR-143-3b和miR-125b-5p提供了有价值的预后信息,但miR-125b-5p与肿瘤标志物CA15-3的组合可提高BC检测的敏感性,值得进一步的验证研究加以考虑。

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