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炎性乳腺癌的基因组和表达分析。

Genomic and expression analysis of microdissected inflammatory breast cancer.

机构信息

Departments of Radiation Oncology, The University of Texas MD Anderson Cancer Center, Houston, TX, USA.

出版信息

Breast Cancer Res Treat. 2013 Apr;138(3):761-72. doi: 10.1007/s10549-013-2501-6. Epub 2013 Apr 9.

Abstract

Inflammatory breast cancer (IBC) is a unique clinical entity characterized by rapid onset of erythema and swelling of the breast often without an obvious breast mass. Many studies have examined and compared gene expression between IBC and non-IBC (nIBC), repeatedly finding clusters associated with receptor subtype, but no consistent gene signature associated with IBC has been validated. Here we compared microdissected IBC tumor cells to microdissected nIBC tumor cells matched based on estrogen and HER-2/neu receptor status. Gene expression analysis and comparative genomic hybridization were performed. An IBC gene set and genomic set were identified using a training set and validated on the remaining data. The IBC gene set was further tested using data from IBC consortium samples and publicly available data. Receptor driven clusters were identified in IBC; however, no IBC-specific gene signature was identified. Fifteen genes were correlated between increased genomic copy number and gene overexpression data. An expression-guided gene set upregulated in the IBC training set clustered the validation set into two clusters independent of receptor subtype but segregated only 75 % of samples in each group into IBC or nIBC. In a larger consortium cohort and in published data, the gene set failed to optimally enrich for IBC samples. However, this gene set had a high negative predictive value for excluding the diagnosis of IBC in publicly available data (100 %). An IBC enriched genomic data set accurately identified 10/16 cases in the validation data set. Even with microdissection, no IBC-specific gene signature distinguishes IBC from nIBC. Using microdissected data, a validated gene set was identified that is associated with IBC tumor cells. Inflammatory breast cancer comparative genomic hybridization data are presented, but a validated genomic data set that identifies IBC is not demonstrated.

摘要

炎性乳腺癌(IBC)是一种独特的临床实体,其特征为乳腺迅速出现红斑和肿胀,通常没有明显的乳腺肿块。许多研究已经检查并比较了 IBC 和非炎性乳腺癌(nIBC)之间的基因表达,反复发现与受体亚型相关的聚类,但尚未验证与 IBC 相关的一致基因特征。在这里,我们将微切割的 IBC 肿瘤细胞与根据雌激素和 HER-2/neu 受体状态匹配的微切割的 nIBC 肿瘤细胞进行比较。进行了基因表达分析和比较基因组杂交。使用训练集确定了 IBC 基因集和基因组集,并在其余数据上进行了验证。使用 IBC 联盟样本和公开可用数据进一步测试了 IBC 基因集。在 IBC 中鉴定了受体驱动的聚类;然而,没有鉴定出 IBC 特异性的基因特征。在基因表达上调的 IBC 训练集中,有 15 个基因与基因过表达数据的基因拷贝数增加相关。基于受体的聚类在 IBC 中鉴定出;然而,没有鉴定出 IBC 特异性的基因特征。在 IBC 训练集中上调的表达指导基因集将验证集聚类为两个独立于受体亚型的聚类,但仅将每个组中的 75%的样本分为 IBC 或 nIBC。在更大的联盟队列和已发表的数据中,基因集未能最佳富集 IBC 样本。然而,该基因集在公开可用数据中排除 IBC 诊断的阴性预测值很高(100%)。在验证数据集中,IBC 富集基因组数据集准确识别了 10/16 例。即使进行了微切割,也没有能够将 IBC 与 nIBC 区分开来的 IBC 特异性基因特征。使用微切割数据,鉴定出一个经过验证的与 IBC 肿瘤细胞相关的基因集。提供了炎性乳腺癌比较基因组杂交数据,但未证明存在可识别 IBC 的经过验证的基因组数据集。

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Genomic and expression analysis of microdissected inflammatory breast cancer.炎性乳腺癌的基因组和表达分析。
Breast Cancer Res Treat. 2013 Apr;138(3):761-72. doi: 10.1007/s10549-013-2501-6. Epub 2013 Apr 9.

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