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乳腺癌转移至妇科器官:临床病理和分子特征研究。

Breast cancer metastasis to gynaecological organs: a clinico-pathological and molecular profiling study.

机构信息

Centre for Clinical Research, Faculty of Medicine, The University of Queensland, Brisbane, Australia.

Personalised Medicine, QIMR Berghofer Medical Research Institute, Brisbane, Australia.

出版信息

J Pathol Clin Res. 2019 Jan;5(1):25-39. doi: 10.1002/cjp2.118. Epub 2018 Oct 22.

Abstract

Breast cancer metastasis to gynaecological organs is an understudied pattern of tumour spread. We explored clinico-pathological and molecular features of these metastases to better understand whether this pattern of dissemination is organotropic or a consequence of wider metastatic dissemination. Primary and metastatic tumours from 54 breast cancer patients with gynaecological metastases were analysed using immunohistochemistry, DNA copy-number profiling, and targeted sequencing of 386 cancer-related genes. The median age of primary tumour diagnosis amongst patients with gynaecological metastases was significantly younger compared to a general breast cancer population (46.5 versus 60 years; p < 0.0001). Median age at metastatic diagnosis was 54.4, time to progression was 4.8 years (range 0-20 years), and survival following a diagnosis of metastasis was 1.95 years (range 0-18 years). Patients had an average of five involved sites (most frequently ovary, fallopian tube, omentum/peritoneum), with fewer instances of spread to the lungs, liver, or brain. Invasive lobular histology and luminal A-like phenotype were over-represented in this group (42.8 and 87.5%, respectively) and most patients had involved axillary lymph nodes (p < 0.001). Primary tumours frequently co-expressed oestrogen receptor cofactors (GATA3, FOXA1) and harboured amplifications at 8p12, 8q24, and 11q13. In terms of phenotype conversion, oestrogen receptor status was generally maintained in metastases, FOXA1 increased, and expression of progesterone receptor, androgen receptor, and GATA3 decreased. ESR1 and novel AR mutations were identified. Metastasis to gynaecological organs is a complication frequently affecting young women with invasive lobular carcinoma and luminal A-like breast cancer, and hence may be driven by sustained hormonal signalling. Molecular analyses reveal a spectrum of factors that could contribute to de novo or acquired resistance to therapy and disease progression.

摘要

乳腺癌转移至妇科器官是一种研究较少的肿瘤扩散模式。我们探讨了这些转移的临床病理和分子特征,以更好地了解这种扩散模式是器官趋向性的还是广泛转移扩散的结果。我们使用免疫组织化学、DNA 拷贝数分析和 386 个癌症相关基因的靶向测序分析了 54 名患有妇科转移的乳腺癌患者的原发和转移肿瘤。患有妇科转移的患者的原发肿瘤诊断中位年龄明显低于一般乳腺癌人群(46.5 岁比 60 岁;p<0.0001)。转移性诊断的中位年龄为 54.4 岁,进展时间为 4.8 年(范围 0-20 年),转移后生存时间为 1.95 年(范围 0-18 年)。患者平均有 5 个受累部位(最常见的是卵巢、输卵管、大网膜/腹膜),肺部、肝脏或脑部受累的情况较少。在这组患者中,浸润性小叶癌组织学和腔A型表型过度表达(分别为 42.8%和 87.5%),大多数患者腋窝淋巴结受累(p<0.001)。原发肿瘤经常共表达雌激素受体共因子(GATA3、FOXA1),并在 8p12、8q24 和 11q13 处发生扩增。就表型转化而言,雌激素受体状态在转移中通常得到维持,FOXA1 增加,孕激素受体、雄激素受体和 GATA3 的表达减少。鉴定了 ESR1 和新型 AR 突变。转移至妇科器官是一种常见的并发症,常影响年轻的浸润性小叶癌和腔A型乳腺癌女性,因此可能是由持续的激素信号驱动的。分子分析揭示了一系列可能导致新发生或获得性耐药和疾病进展的因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c80/6317061/c4facdfbe3c8/CJP2-5-25-g001.jpg

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