同步导管原位癌和浸润性乳腺癌中具有可比性的癌症相关突变特征。
Comparable cancer-relevant mutation profiles in synchronous ductal carcinoma in situ and invasive breast cancer.
机构信息
Department of Cancer Genetics, Institute for Cancer Research, Oslo University Hospital, Oslo, Norway.
Institute of Clinical Medicine, Faculty of Medicine, University of Oslo, Oslo, Norway.
出版信息
Cancer Rep (Hoboken). 2020 Jun;3(3):e1248. doi: 10.1002/cnr2.1248. Epub 2020 May 28.
BACKGROUND
Ductal carcinoma in situ (DCIS) comprises a diverse group of preinvasive lesions in the breast and poses a considerable clinical challenge due to lack of markers of progression. Genomic alterations are to a large extent similar in DCIS and invasive carcinomas, although differences in copy number aberrations, gene expression patterns, and mutations exist. In mixed tumors with synchronous invasive breast cancer (IBC) and DCIS, it is still unclear to what extent invasive tumor cells are directly derived from the DCIS cells.
AIM
Our aim was to compare cancer-relevant mutation profiles of different cellular compartments in mixed DCIS/IBC and pure DCIS tumors.
METHODS AND RESULTS
We performed targeted sequencing of 50 oncogenes in microdissected tissue from three different epithelial cell compartments (in situ, invasive, and normal adjacent epithelium) from 26 mixed breast carcinomas. In total, 44 tissue samples (19 invasive, 16 in situ, 9 normal) were subjected to sequencing using the Ion Torrent platform and the AmpliSeq Cancer Hotspot Panel v2. For comparison, 10 additional, pure DCIS lesions were sequenced. Across all mixed samples, we detected 23 variants previously described in cancer. The most commonly affected genes were TP53, PIK3CA, and ERBB2. The PIK3CA:p.H1047R variant was found in nine samples from six patients. Most variants detected in invasive compartments were also found in the corresponding in situ cell compartment indicating a clonal relationship between the tumor stages. A lower frequency of variants were observed in pure DCIS lesions.
CONCLUSION
Similar mutation profiles between in situ and invasive cell compartments indicate a similar origin of the two tumor stages in mixed breast tumors. The lower number of potential driver variants found in pure DCIS compared with the in situ cell compartments of mixed tumors may imply that pure DCIS is captured earlier in the path of progression to invasive disease.
背景
导管原位癌(DCIS)是乳腺中一组不同的浸润前病变,由于缺乏进展标志物,因此具有相当大的临床挑战性。尽管在拷贝数异常、基因表达模式和突变方面存在差异,但 DCIS 和浸润性癌在很大程度上具有相似的基因组改变。在伴有同步浸润性乳腺癌(IBC)和 DCIS 的混合肿瘤中,浸润性肿瘤细胞是否直接来源于 DCIS 细胞尚不清楚。
目的
我们旨在比较混合 DCIS/IBC 和单纯 DCIS 肿瘤不同细胞区室中与癌症相关的突变谱。
方法和结果
我们对 26 例混合乳腺癌中三个不同上皮细胞区室(原位、浸润和正常相邻上皮)的微切割组织进行了 50 个癌基因的靶向测序。总共对 44 个组织样本(19 个浸润性、16 个原位、9 个正常)进行了测序,使用 Ion Torrent 平台和 AmpliSeq Cancer Hotspot Panel v2。为了比较,还对 10 个额外的单纯 DCIS 病变进行了测序。在所有混合样本中,我们检测到了 23 个先前在癌症中描述过的变体。受影响最常见的基因是 TP53、PIK3CA 和 ERBB2。PIK3CA:p.H1047R 变体在六个患者的九个样本中被发现。在侵袭性区室中检测到的大多数变体也在相应的原位细胞区室中被发现,这表明肿瘤分期之间存在克隆关系。在单纯 DCIS 病变中观察到的变体频率较低。
结论
原位和侵袭性细胞区室之间相似的突变谱表明混合乳腺癌中两种肿瘤阶段具有相似的起源。与混合肿瘤的原位细胞区室相比,单纯 DCIS 中发现的潜在驱动变异数量较少,这可能意味着单纯 DCIS 在进展为浸润性疾病的过程中更早被捕获。
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