Vincent-Salomon Anne, Bataillon Guillaume, Djerroudi Lounes
Inserm U934, département de médecine diagnostique et théranostique, service de pathologie, institut Curie, université Paris sciences lettres, 26, rue d'Ulm, 75005 Paris, France.
Département de médecine diagnostique et théranostique, service de pathologie, institut Curie, université Paris sciences lettres, 26, rue d'Ulm, 75005 Paris, France.
Ann Pathol. 2020 Apr;40(2):78-84. doi: 10.1016/j.annpat.2020.02.023. Epub 2020 Mar 30.
Breast cancers occurring in the context of a hereditary mutation of a predisposition gene represent 5 to 10% of all breast cancers, 20 to 25% of which being due to a mutation in the BRCA1 or BRCA2 genes. Authorization to market PARP inhibitors for breast cancer patients with hereditary BRCA1 and 2 mutations has recently been obtained. Given the annual frequency of breast cancer, morphological identification could facilitate the patient care process to limit the search for BRCA1 and 2 mutations to patients whose tumors have very specific characteristics. However, only a few morphological features have been recognized and differ depending on the mutated genes. Breast cancer occurring as part of a mutation in the BRCA1 gene is in 85% of cases of high-grade non-specific type invasive carcinomas with very limited contours, contain numerous lymphocytes in the stroma and are of triple-negative phenotype. Carcinomas associated with mutations in the BRCA2 genes and genes more recently recognized as associated with a risk of development of breast cancer (CHECK2, BMPR1A, BRIP1, PALB2, MUTYH) are most often non-specific invasive carcinomas, although other histological types are possible, grade III, luminal B phenotype. Breast cancer occurring in the context of a constitutional mutation of TP53 occurs in women under 35 years old are of non-specific histological type and with an amplification of HER2 in two thirds of the cases. Those associated with a PTEN mutation are readily of the apocrine type. Finally, very rarely, certain lobular-type breast cancers can occur in the context of a constitutional mutation of the CDH1 gene, which codes for the protein E-cadherin. The morphological and phenotypic characteristics may suggest to the pathologist a carcinoma of the breast occurring in a context of hereditary mutation. However, at the present time the only situations where a morphological sorting makes it possible to accelerate the genetic analysis are those of an invasive carcinoma of non-specific type of triple-negative phenotype in a woman of less than 50 years or that of a diagnosis of HER2 breast cancer amplified in a woman under 31 years of age (Chompret criteria). Family background and personal history are of great importance in the genetic counseling indication decision trees. Unfortunately, to date, no quality antibody has been developed against BRCA1 and 2 to help the pathologist identify hereditary cases. The immunohistochemical analysis of RAD51 could facilitate the identification of tumors possibly sensitive to PARP inhibitors. Progress to identify hereditary cancers is expected thanks to the development of artificial intelligence algorithms from digitized histological slides.
由易感基因的遗传性突变引发的乳腺癌占所有乳腺癌的5%至10%,其中20%至25%归因于BRCA1或BRCA2基因的突变。PARP抑制剂已获批准用于治疗患有遗传性BRCA1和2突变的乳腺癌患者。鉴于乳腺癌的年发病频率,形态学识别有助于优化患者护理流程,将BRCA1和2突变的检测局限于具有非常特殊特征的肿瘤患者。然而,目前仅识别出少数形态学特征,且这些特征因突变基因而异。由BRCA1基因突变引发的乳腺癌,85%为高级别非特异性浸润性癌,边界非常局限,间质中含有大量淋巴细胞,呈三阴性表型。与BRCA2基因以及最近被认为与乳腺癌发生风险相关的基因(CHECK2、BMPR1A、BRIP1、PALB2、MUTYH)突变相关的癌,大多为非特异性浸润性癌,不过也可能有其他组织学类型,为三级管腔B型表型。由TP53基因的体质性突变引发的乳腺癌发生在35岁以下女性中,组织学类型非特异性,三分之二的病例HER2呈扩增状态。与PTEN突变相关的乳腺癌多为大汗腺型。最后,非常罕见的是,某些小叶型乳腺癌可发生于编码E-钙黏蛋白的CDH1基因的体质性突变背景下。形态学和表型特征可能会提示病理学家该乳腺癌发生于遗传性突变背景下。然而,目前形态学分类能够加速基因分析的唯一情况是,50岁以下女性的非特异性三阴性浸润性癌,或31岁以下女性诊断为HER2扩增型乳腺癌(乔普雷标准)。家族背景和个人病史在遗传咨询指征决策树中至关重要。不幸的是,迄今为止,尚未开发出针对BRCA1和2的优质抗体来帮助病理学家识别遗传性病例。RAD51的免疫组化分析可能有助于识别可能对PARP抑制剂敏感的肿瘤。随着基于数字化组织学切片的人工智能算法的发展,有望在识别遗传性癌症方面取得进展。
