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一种与乳腺癌患者胸水中转移细胞相关的基因表达特征。

A gene expression signature associated with metastatic cells in effusions of breast carcinoma patients.

作者信息

Dupont Virginie N, Gentien David, Oberkampf Marine, De Rycke Yann, Blin Nathalie

机构信息

UMR144 CNRS, Research Division, Institut Curie, Paris, France.

出版信息

Int J Cancer. 2007 Sep 1;121(5):1036-46. doi: 10.1002/ijc.22775.

Abstract

Malignant effusion in invasive breast carcinoma is associated with poor prognosis. To decipher molecular events leading to metastasis and to identify reliable markers for targeted therapies are of crucial need. Therefore, we have used cDNA microarrays to delineate molecular signatures associated with metastasis and relapse in breast carcinoma effusions. Taking advantage of an immunomagnetic method, we have purified to homogeneity EpCAM-positive cells from 34 malignant effusions. Immunopurified cells represented as much as 10% of the whole cell fraction and their epithelial and carcinoma features were confirmed by immunofluorescence labeling. Gene expression profiles of 19 immunopurified effusion samples, were analyzed using human pan-genomic microarrays, and compared with those of 4 corresponding primary tumors, 8 breast carcinoma effusion-derived cell lines, and 4 healthy mammary tissues. Principal component and multiple clustering analyses of microarray data, clearly identified distinctive molecular portraits corresponding to the 4 categories of specimens. Of uppermost interest, effusion samples were arranged in 2 subsets on the basis of their gene expression patterns. The first subset partly shares a gene expression signature with the different cell lines, and overexpresses CD24, CD44 and epithelial cytokeratins 8,18,19. The second subset overexpresses markers related to aggressive invasive carcinoma (uPA receptor, S100A4, vimentin, CXCR4). These findings demonstrate the importance of using pure cell fractions to accurately decipher in silico gene expression of clinical specimens. Further studies will lead to the identification of genes of oustanding importance to diagnose malignant effusion, predict survival and tailor appropriate therapies to the metastatic effusion disease in breast carcinoma patients.

摘要

浸润性乳腺癌中的恶性胸腔积液与预后不良相关。解读导致转移的分子事件并确定靶向治疗的可靠标志物至关重要。因此,我们使用cDNA微阵列来描绘与乳腺癌胸腔积液转移和复发相关的分子特征。利用免疫磁珠法,我们从34例恶性胸腔积液中纯化出了均一的EpCAM阳性细胞。免疫纯化的细胞占全细胞组分的10%,其上皮和癌特征通过免疫荧光标记得以证实。使用人类全基因组微阵列分析了19个免疫纯化的胸腔积液样本的基因表达谱,并与4个相应的原发性肿瘤、8个乳腺癌胸腔积液来源的细胞系以及4个健康乳腺组织的基因表达谱进行了比较。微阵列数据的主成分分析和多重聚类分析清楚地确定了与4类标本相对应的独特分子图谱。最令人感兴趣的是,胸腔积液样本根据其基因表达模式被分为两个亚组。第一个亚组部分与不同细胞系共享基因表达特征,并过度表达CD24、CD44以及上皮细胞角蛋白8、18、19。第二个亚组过度表达与侵袭性癌相关的标志物(尿激酶型纤溶酶原激活物受体、S100A4、波形蛋白、CXCR4)。这些发现证明了使用纯细胞组分来准确解读临床标本的电子基因表达的重要性。进一步的研究将有助于鉴定对诊断恶性胸腔积液、预测生存以及为乳腺癌患者的转移性胸腔积液疾病制定合适治疗方案具有极其重要意义的基因。

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