PIK3CA mutations are common in lobular carcinoma in situ, but are not a biomarker of progression.

IF 5.6 1区医学 Q1 ONCOLOGY

Breast Cancer Research Pub Date : 2017-01-17 DOI:10.1186/s13058-016-0789-y

Vandna Shah, Salpie Nowinski, Dina Levi, Irek Shinomiya, Narda Kebaier Ep Chaabouni, Cheryl Gillett, Anita Grigoriadis, Trevor A Graham, Rebecca Roylance, Michael A Simpson, Sarah E Pinder, Elinor J Sawyer

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Abstract

Background: Lobular carcinoma in situ (LCIS) is a non-invasive breast lesion that is typically found incidentally on biopsy and is often associated with invasive lobular carcinoma (ILC). LCIS is considered by some to be a risk factor for future breast cancer rather than a true precursor lesion. The aim of this study was to identify genetic changes that could be used as biomarkers of progression of LCIS to invasive disease using cases of pure LCIS and comparing their genetic profiles to LCIS which presented contemporaneously with associated ILC, on the hypothesis that the latter represents LCIS that has already progressed.

Methods: Somatic copy number aberrations (SCNAs) were assessed by SNP array in three subgroups: pure LCIS, LCIS associated with ILC and the paired ILC. In addition exome sequencing was performed on seven fresh frozen samples of LCIS associated with ILC, to identify recurrent somatic mutations.

Results: The copy number profiles of pure LCIS and LCIS associated with ILC were almost identical. However, four SCNAs were more frequent in ILC than LCIS associated with ILC, including gain/amplification of CCND1. CCND1 protein over-expression assessed by immunohistochemical analysis in a second set of samples from 32 patients with pure LCIS and long-term follow up, was associated with invasive recurrence (P = 0.02, Fisher's exact test). Exome sequencing revealed that PIK3CA mutations were as frequent as CDH1 mutations in LCIS, but were not a useful biomarker of LCIS progression as they were as frequent in pure LCIS as in LCIS associated with ILC. We also observed heterogeneity of PIK3CA mutations and evidence of sub-clonal populations in LCIS irrespective of whether they were associated with ILC.

Conclusions: Our data shows that pure LCIS and LCIS co-existing with ILC have very similar SCNA profiles, supporting the hypothesis that LCIS is a true precursor lesion. We have provided evidence that over-expression of CCND1 may identify a subgroup of patients with pure LCIS who are more likely to develop invasive disease, in contrast to PIK3CA mutations, which occur too early in lobular tumorigenesis to be informative.

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PIK3CA突变在小叶原位癌中很常见，但不是进展的生物标志物。

背景：小叶原位癌（LCIS）是一种非浸润性乳腺病变，通常在活检中偶然发现，通常与浸润性小叶癌（ILC）相关。LCIS被一些人认为是未来乳腺癌的危险因素，而不是真正的前驱病变。本研究的目的是通过使用纯LCIS病例，并将其遗传谱与与相关ILC同时出现的LCIS进行比较，以确定可作为LCIS进展为侵袭性疾病的生物标志物的遗传变化，假设后者代表已经进展的LCIS。方法：采用单核苷酸多态性（SNP）阵列对纯LCIS、伴ILC LCIS和配对ILC LCIS三个亚组的体细胞拷贝数畸变（SCNAs）进行评估。此外，对7个与ILC相关的LCIS新鲜冷冻样本进行外显子组测序，以确定复发性体细胞突变。结果：LCIS与LCIS合并ILC的拷贝数谱基本相同。然而，四种scna在ILC中比与ILC相关的LCIS更频繁，包括CCND1的增益/扩增。在32例LCIS患者和长期随访的第二组样本中，通过免疫组织化学分析评估CCND1蛋白过表达与侵袭性复发相关（P = 0.02， Fisher精确检验）。外显子组测序显示，PIK3CA突变在LCIS中与CDH1突变一样频繁，但不是LCIS进展的有用生物标志物，因为它们在纯LCIS中与在与ILC相关的LCIS中一样频繁。我们还观察到PIK3CA突变的异质性和LCIS中亚克隆群体的证据，无论它们是否与ILC相关。结论：我们的数据显示，单纯LCIS和LCIS合并ILC具有非常相似的SCNA谱，支持LCIS是真正的前驱病变的假设。我们提供的证据表明，与PIK3CA突变相比，CCND1的过表达可能会识别出一组更容易发展为侵袭性疾病的纯LCIS患者，PIK3CA突变在小叶肿瘤发生中发生得太早，无法提供信息。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Breast Cancer Research 医学-肿瘤学

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期刊介绍： Breast Cancer Research is an international, peer-reviewed online journal, publishing original research, reviews, editorials and reports. Open access research articles of exceptional interest are published in all areas of biology and medicine relevant to breast cancer, including normal mammary gland biology, with special emphasis on the genetic, biochemical, and cellular basis of breast cancer. In addition to basic research, the journal publishes preclinical, translational and clinical studies with a biological basis, including Phase I and Phase II trials.