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Different gene expression patterns in invasive lobular and ductal carcinomas of the breast

机译:乳腺浸润性小叶癌和导管癌的不同基因表达模式

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Invasive ductal carcinoma (IDC) and invasive lobular carcinoma (ILC) are the two major histological types of breast cancer worldwide. Whereas IDC incidence has remained stable, ILC is the most rapidly increasing breast cancer phenotype in the United States and Western Europe. It is not clear whether IDC and ILC represent molecularly distinct entities and what genes might be involved in the development of these two phenotypes. We conducted comprehensive gene expression profiling studies to address these questions. Total RNA from 21 ILCs, 38 IDCs, two lymph node metastases, and three normal tissues were amplified and hybridized to similar to42,000 clone cDNA microarrays. Data were analyzed using hierarchical clustering algorithms and statistical analyses that identify clifferentially expressed genes (significance analysis of microarrays) and minimal subsets of genes (prediction analysis for microarrays) that succinctly distinguish ILCs and IDCs. Eleven of 21 (52%) of the ILCs ("typical" ILCs) clustered together and displayed different gene expression profiles from IDCs, whereas the other ILCs ("ductal-like" ILCs) were distributed between different IDC subtypes. Many of the differentially expressed genes between ILCs and IDCs code for proteins involved in cell adhesion/motility, lipid/fatty acid transport and metabolism, immune/defense response, and electron transport. Many genes that distinguish typical and ductal-like ILCs are involved in regulation of cell growth and immune response. Our data strongly suggest that over half the ILCs differ from IDCs not only in histological and clinical features but also in global transcription programs. The remaining ILCs closely resemble IDCs in their transcription patterns. Further studies are needed to explore the differences between ILC molecular subtypes and to determine whether they require different therapeutic strategies.
机译:浸润性导管癌(IDC)和浸润性小叶癌(ILC)是全世界乳腺癌的两种主要组织学类型。 IDC发病率保持稳定,而ILC是美国和西欧增长最快的乳腺癌表型。目前尚不清楚IDC和ILC是否代表分子上不同的实体,以及哪些基因可能参与这两个表型的发展。我们进行了全面的基因表达谱研究,以解决这些问题。扩增了来自21个ILC,38个IDC,两个淋巴结转移和三个正常组织的总RNA,并将其与相似的42,000个克隆cDNA微阵列杂交。使用分层聚类算法和统计分析对数据进行分析,这些数据可识别出微弱表达的基因(微阵列的重要性分析)和能简洁地区分ILC和IDC的最小基因子集(微阵列的预测分析)。 21个ILC(“典型” ILC)中的11个(“典型” ILC)聚集在一起并显示出与IDC不同的基因表达谱,而其他ILC(“导管样” ILC)则分布在不同的IDC亚型之间。 ILC和IDC之间的许多差异表达基因编码涉及细胞粘附/运动,脂质/脂肪酸运输和代谢,免疫/防御反应以及电子运输的蛋白质。区分典型和导管样ILC的许多基因都参与细胞生长和免疫应答的调节。我们的数据强烈表明,超过一半的ILC与IDC不仅在组织学和临床特征上不同,而且在全球转录程序上也不同。其余的ILC在转录模式上与IDC非常相似。需要进一步研究以探索ILC分子亚型之间的差异,并确定它们是否需要不同的治疗策略。

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