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首页> 外文期刊>Breast cancer research and treatment. >High-resolution genomic profiling of male breast cancer reveals differences hidden behind the similarities with female breast cancer.
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High-resolution genomic profiling of male breast cancer reveals differences hidden behind the similarities with female breast cancer.

机译:男性乳腺癌的高分辨率基因组分析揭示了与女性乳腺癌相似之处背后隐藏的差异。

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Male breast cancer (MBC) is extremely rare and poorly characterized on the molecular level. Using high-resolution genomic data, we aimed to characterize MBC by genomic imbalances and to compare it with female breast cancer (FBC), and further to investigate whether the genomic profiles hold any prognostic information. Fifty-six fresh frozen MBC tumors were analyzed using high-resolution tiling BAC arrays. Significant regions in common between cases were assessed using Genomic Identification of Significant Targets in Cancer (GISTIC) analysis. A publicly available genomic data set of 359 FBC tumors was used for reference purposes. The data revealed a broad pattern of aberrations, confirming that MBC is a heterogeneous tumor type. Genomic gains were more common in MBC than in FBC and often involved whole chromosome arms, while losses of genomic material were less frequent. The most common aberrations were similar between the genders, but high-level amplifications were more common in FBC. We identified two genomic subgroups among MBCs; male-complex and male-simple. The male-complex subgroup displayed striking similarities with the previously reported luminal-complex FBC subgroup, while the male-simple subgroup seems to represent a new subgroup of breast cancer occurring only in men. There are many similarities between FBC and MBC with respect to genomic imbalances, but there are also distinct differences as revealed by high-resolution genomic profiling. MBC can be divided into two comprehensive genomic subgroups, which may be of prognostic value. The male-simple subgroup appears notably different from any genomic subgroup so far defined in FBC.
机译:男性乳腺癌(MBC)极为罕见,在分子水平上的特征也很差。我们使用高分辨率基因组数据,旨在通过基因组失衡来表征MBC,并将其与女性乳腺癌(FBC)进行比较,并进一步调查基因组谱是否具有任何预后信息。使用高分辨率切片BAC阵列分析了56例新鲜冷冻的MBC肿瘤。使用癌症中重要靶点的基因组鉴定(GISTIC)分析评估病例之间共有的重要区域。使用359个FBC肿瘤的公开基因组数据集作为参考。数据揭示了畸变的广泛模式,证实了MBC是异质性肿瘤类型。 MBC中的基因组增益比FBC中的更为常见,并且通常涉及整个染色体臂,而基因组物质的损失则较少。性别之间最常见的像差相似,但在FBC中高水平的放大更为常见。我们在MBC中确定了两个基因组亚组。男性复杂和男性简单。男性复杂亚组与先前报道的管腔复杂FBC亚组表现出惊人的相似性,而男性简单亚组似乎代表了仅在男性中发生的乳腺癌新亚组。 FBC和MBC在基因组失衡方面有许多相似之处,但高分辨率基因组分析也显示出明显的差异。 MBC可分为两个全面的基因组亚组,可能具有预后价值。雄性简单亚组似乎与迄今为止在FBC中定义的任何基因组亚组明显不同。

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