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Lymphovascular invasion and histologic grade are associated with specific genomic profiles in invasive carcinomas of the breast

机译:淋巴管浸润和组织学分级与乳腺浸润癌的特定基因组谱相关

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摘要

Lymphovascular invasion (LVI) and histologic grade are clinical parameters of high prognostic value in breast cancer and indicate the level of tumor aggressiveness. Many studies have focused on the association of breast cancer subtypes with gene expression and chromosomal profiles, but considerably less genomic information is available regarding traditional prognostic factors such as histologic grade and LVI. We studied by array-CGH a group of 57 invasive ductal carcinomas of the breast to outline the DNA copy number aberration (CNA) profile linked to high histologic grades and LVI. Selected CNAs were validated using real-time quantitative PCR (qPCR). Furthermore, gene expression analysis was performed in a subset of 32 of these tumors, and findings were integrated with array-CGH data. Our findings indicated an accumulation of genomic alterations in high-grade breast tumors compared to low-grade samples. Grade III tumors showed higher number of CNAs and larger aberrations than low-grade tumors and displayed a wide range of chromosomal aberrations, which were mainly 5p, 8q, 10p, 17q12, and 19 gains, and 3p, 4, 5q proximal, 9p, 11p, 18q, and 21 losses. The presence of LVI, a well-established prognostic marker, was not significantly associated with increased genomic instability in comparison to breast tumors negative for LVI, considering the total number of chromosomal alterations. However, a slightly increase in the frequency of specific alterations could be detected in LVI-positive group, such as gains at 5p, 16p, 17q12, and 19, and losses at 8p, 11q, 18q, and 21. Three newly reported small-scale rearrangements were detected in high-risk tumors (LVI-positive grade III) harboring putative breast cancer genes (amplicons at 4q13.3 and 11p11.2, and a deletion at 12p12.3). Furthermore, gene expression analysis uncovered networks highlighting S100A8, MMP1, and MED1 as promising candidate genes involved in high-grade and LVI-positive tumors. In summary, a group of genomic regions could be associated with high-risk tumors, and expression analysis pinpointed candidate genes deserving further investigation. The data has shed some light on the molecular players involved in two highly relevant prognostic factors and may further add to the understanding of the mechanisms of breast cancer aggressiveness.Electronic supplementary materialThe online version of this article (doi:10.1007/s13277-014-2786-z) contains supplementary material, which is available to authorized users.
机译:淋巴管浸润(LVI)和组织学分级是乳腺癌的高预后价值的临床参数,并表明肿瘤的侵袭性水平。许多研究集中在乳腺癌亚型与基因表达和染色体谱的关系上,但是关于传统预后因素(如组织学等级和LVI)的基因组信息却很少。我们通过阵列CGH研究了一组57个乳腺浸润性导管癌,以概述与高组织学等级和LVI相关的DNA拷贝数畸变(CNA)概况。使用实时定量PCR(qPCR)验证选定的CNA。此外,在这些肿瘤的32个子集中进行了基因表达分析,并将发现结果与阵列CGH数据整合在一起。我们的发现表明,与低度样品相比,高度乳腺肿瘤中基因组改变的积累。与低度肿瘤相比,III级肿瘤的CNA数量更多,畸变更大,并且染色体畸变范围很广,主要是5p,8q,10p,17q12和19增益,以及3p,4、5q近端,9p, 11p,18q和21损失。考虑到染色体改变的总数,与公认的LVI阴性的乳腺肿瘤相比,LVI是一种公认​​的预后标志物,与基因组不稳定性的增加没有显着相关。但是,在LVI阳性组中,可以检测到特定变化的频率略有增加,例如在5p,16p,17q12和19时增益,而在8p,11q,18q和21时损耗。在携带推定的乳腺癌基因(4q13.3和11p11.2的扩增子,以及12p12.3的缺失)的高风险肿瘤(LVI阳性III级)中检测到了标度重排。此外,基因表达分析发现网络突出显示了S100A8,MMP1和MED1是参与高级别和LVI阳性肿瘤的有前途的候选基因。总之,一组基因组区域可能与高危肿瘤有关,表达分析确定了候选基因,值得进一步研究。数据为涉及两个高度相关的预后因素的分子因素提供了一些线索,并可能进一步加深对乳腺癌侵袭性机制的了解。电子补充材料本文的在线版本(doi:10.1007 / s13277-014-2786 -z)包含补充材料,授权用户可以使用。

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