Queensland Institute of Medical Research, Brisbane, Australia.
Breast Cancer Res Treat. 2010 Oct;123(3):661-77. doi: 10.1007/s10549-009-0653-1. Epub 2009 Dec 4.
Extensive expression profiling studies have shown that sporadic breast cancer is composed of five clinically relevant molecular subtypes. However, although BRCA1-related tumours are known to be predominantly basal-like, there are few published data on other classes of familial breast tumours. We analysed a cohort of 75 BRCA1, BRCA2 and non-BRCA1/2 breast tumours by gene expression profiling and found that 74% BRCA1 tumours were basal-like, 73% of BRCA2 tumours were luminal A or B, and 52% non-BRCA1/2 tumours were luminal A. Thirty-four tumours were also analysed by single nucleotide polymorphism-comparative genomic hybridization (SNP-CGH) arrays. Copy number data could predict whether a tumour was basal-like or luminal with high accuracy, but could not predict its mutation class. Basal-like BRCA1 and basal-like non-BRCA1 tumours were very similar, and contained the highest number of chromosome aberrations. We identified regions of frequent gain containing potential driver genes in the basal (8q and 12p) and luminal A tumours (1q and 17q). Regions of homozygous loss associated with decreased expression of potential tumour suppressor genes were also detected, including in basal tumours (5q and 9p), and basal and luminal tumours (10q). This study highlights the heterogeneity of familial tumours and the clinical consequences for treatment and prognosis.
广泛的表达谱研究表明,散发性乳腺癌由五个临床相关的分子亚型组成。然而,尽管已知 BRCA1 相关肿瘤主要是基底样的,但关于其他家族性乳腺癌肿瘤类别的发表数据很少。我们通过基因表达谱分析了 75 例 BRCA1、BRCA2 和非 BRCA1/2 乳腺癌肿瘤,发现 74%的 BRCA1 肿瘤为基底样,73%的 BRCA2 肿瘤为 luminal A 或 B,52%的非 BRCA1/2 肿瘤为 luminal A。还对 34 例肿瘤进行了单核苷酸多态性比较基因组杂交(SNP-CGH)阵列分析。拷贝数数据可以高度准确地预测肿瘤是否为基底样或 luminal 型,但不能预测其突变类型。BRCA1 基底样和非 BRCA1 基底样肿瘤非常相似,并且包含最多的染色体异常。我们在基底样(8q 和 12p)和 luminal A 肿瘤(1q 和 17q)中鉴定了包含潜在驱动基因的频繁增益区域。还检测到与潜在肿瘤抑制基因表达降低相关的纯合性缺失区域,包括在基底样肿瘤(5q 和 9p)以及基底样和 luminal 肿瘤(10q)中。这项研究强调了家族性肿瘤的异质性及其对治疗和预后的临床后果。
