Halvorsen Ann Rita, Helland Åslaug, Gromov Pavel, Wielenga Vera Timmermans, Talman Maj-Lis Møller, Brunner Nils, Sandhu Vandana, Børresen-Dale Anne-Lise, Gromova Irina, Haakensen Vilde D
Department of Cancer Genetics, Institute for Cancer Research, The Norwegian Radium Hospital, Oslo University Hospital, Norway.
Department of Oncology, The Norwegian Radium Hospital, Oslo University Hospital, Norway.
Mol Oncol. 2017 Feb;11(2):220-234. doi: 10.1002/1878-0261.12025. Epub 2016 Dec 12.
It has been hypothesized based on accumulated data that a class of small noncoding RNAs, termed microRNAs, are key factors in intercellular communication. Here, microRNAs present in interstitial breast tumor fluids have been analyzed to identify relevant markers for a diagnosis of breast cancer and to elucidate the cross-talk that exists among cells in a tumor microenvironment. Matched tumor interstitial fluid samples (TIF, n = 60), normal interstitial fluid samples (NIF, n = 51), corresponding tumor tissue specimens (n = 54), and serum samples (n = 27) were collected from patients with breast cancer, and detectable microRNAs were analyzed and compared. In addition, serum data from 32 patients with breast cancer and 22 healthy controls were obtained for a validation study. To identify potential serum biomarkers of breast cancer, first the microRNA profiles of TIF and NIF samples were compared. A total of 266 microRNAs were present at higher level in the TIF samples as compared to normal counterparts. Sixty-one of these microRNAs were present in > 75% of the serum samples and were subsequently tested in a validation set. Seven of the 61 microRNAs were associated with poor survival, while 23 were associated with the presence of immune cells and adipocytes. To our knowledge, these data demonstrate for the first time that profiling of microRNAs in TIF can identify novel biomarkers for the prognostic classification and detection of breast cancer. In addition, the present findings demonstrate that microRNAs may represent the cross-talk that occurs between tumor cells and their surrounding stroma.
基于积累的数据推测,一类被称为微小RNA的小非编码RNA是细胞间通讯的关键因素。在此,对乳腺肿瘤间质液中存在的微小RNA进行了分析,以确定乳腺癌诊断的相关标志物,并阐明肿瘤微环境中细胞间存在的相互作用。从乳腺癌患者中收集了匹配的肿瘤间质液样本(TIF,n = 60)、正常间质液样本(NIF,n = 51)、相应的肿瘤组织标本(n = 54)和血清样本(n = 27),并对可检测的微小RNA进行了分析和比较。此外,还获得了32例乳腺癌患者和22例健康对照的血清数据用于验证研究。为了确定乳腺癌潜在的血清生物标志物,首先比较了TIF和NIF样本的微小RNA谱。与正常样本相比,TIF样本中共有266种微小RNA的水平更高。其中61种微小RNA存在于>75%的血清样本中,随后在验证集中进行了检测。这61种微小RNA中有7种与不良生存相关,23种与免疫细胞和脂肪细胞的存在相关。据我们所知,这些数据首次证明,TIF中微小RNA的分析可以识别用于乳腺癌预后分类和检测的新型生物标志物。此外,目前的研究结果表明,微小RNA可能代表肿瘤细胞与其周围基质之间发生的相互作用。
