乳腺浸润性小叶癌的E-cadherin突变情况与预后

IF 7.1 1区 医学 Q1 PATHOLOGY
Lounes Djerroudi , Amel Bendali , Laetitia Fuhrmann , Camille Benoist , Gaelle Pierron , Julien Masliah-Planchon , Yann Kieffer , Matthieu Carton , Jean-Christophe Tille , Joanna Cyrta , Toulsie Ramtohul , Claire Bonneau , Martial Caly , Victor Renault , François-Clément Bidard , Fatima Mechta-Grigoriou , Anne Vincent-Salomon
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引用次数: 0

摘要

浸润性小叶癌(ILC)的特点是E-cadherin表达缺失和CDH1基因失活。目前,这种肿瘤类型的诊断重现性并不理想,如果能更好地了解其组织分子和临床异质性,就能提高诊断重现性。我们对长期随访(中位数:9.5 年)的 251 例原发性 ILC 进行了回顾性系列研究,分析了 CDH1 突变的存在、类型或位置、E-cadherin 表达与临床病理特征(包括预后)之间的关系。通过对冷冻肿瘤样本进行 RNA 测序,确定了 E-cadherin(CDH1)基因的突变状态。使用针对细胞内结构域(克隆 4A2C7)和细胞外结构域(克隆 NCH38)的抗体对 E-cadherin进行免疫组化(IHC)。还对 E-cadherin弥漫阳性病例中 p120 和 β-catenin 的 IHC 表达进行了评估。通过 IHC 鉴定出 E-cadherin 膜表达的三种主要模式,两个克隆之间有很好的一致性(总体一致性:83.8%,Kappa 0.67):无效/灶性表达(≤10%)(72.8%,NCH38 为 83.8%)、异质性表达(11-89%)(4A2C7 为 19.2%,NCH38 为 6.9%)和弥漫性表达(≥90%)(4A2C7 为 8%,NCH38 为 9.3%)。E-cadherin膜表达即使存在,也是异常的(标记不完整和/或强度降低)。在 21% 的病例中,E-cadherin 弥漫表达的 ILC 显示出异常的 β-catenin 或 p120-catenin 染色。有趣的是,这些E-cadherin弥漫表达病例的CDH1突变率与E-cadherin无效/病灶病例一样高(70%),但却富含非截断突变。关于CDH1突变位置,胞质内结构域突变与两种抗体的E-cadherin IHC表型不同有关(4A2C7 ≤10% / NCH38 ≥10%)。临床病理相关性分析发现,在E-cadherin无效/病灶的ILC病例中,基质数量(与肿瘤细胞性成反比)和TIL数量较少。此外,CDH1截短突变与放射组织学大小不一致有关,并在多变量生存分析中被确定为转移风险和乳腺癌相关死亡率方面的独立不良预后因素。总之,我们的研究强调了 CDH1 的精确突变状态在小叶癌的临床、放射学、组织学和表型表达中的重要性。今后在改进 ILC 诊断标准或方法的尝试中,以及在专门针对这种肿瘤类型的临床生物研究中,都应考虑到这些发现。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
E-Cadherin Mutational Landscape and Outcomes in Breast Invasive Lobular Carcinoma

Invasive lobular carcinomas (ILC) are characterized by the loss of E-cadherin expression and CDH1 gene inactivation. Diagnostic reproducibility for this tumor type is currently suboptimal and could be improved by a better understanding of its histomolecular and clinical heterogeneity. We have analyzed the relationship between the presence, type, or position of CDH1 mutations, E-cadherin expression, and clinicopathological features (including outcome) in a retrospective series of 251 primary ILC with a long follow-up (median: 9.5 years). The mutational status of E-cadherin gene (CDH1) was determined by RNA sequencing from frozen tumor samples. E-cadherin immunohistochemistry (IHC) was performed with antibodies directed against the intracellular domain (clone 4A2C7) and the extracellular domain (clone NCH38). IHC expression of p120 and β-catenin was also assessed in E-cadherin diffusely positive cases. Three major patterns of E-cadherin membrane expression were identified by IHC, with good agreement between the 2 clones (overall concordance: 83.8%, Kappa 0.67): null/focal expression (≤10%) (72.8% of cases for 4A2C7 and 83.8% for NCH38), heterogeneous expression (11%-89%) (19.2% of cases for 4A2C7 and 6.9% for NCH38), and diffuse expression (≥90%) (8% of cases for 4A2C7 and 9.3% for NCH38). E-cadherin membranous expression, when present, was abnormal (incomplete labeling and/or reduced intensity). ILC with diffuse E-cadherin expression showed abnormal β-catenin or p120-catenin staining in 21% of cases. Interestingly, these cases with diffusely expressed E-cadherin had a CDH1 mutation rate as high as the E-cadherin null/focal cases (∼70%) but were enriched in nontruncating mutations. Regarding CDH1 mutation location, intracytoplasmic domain mutations correlated with a divergent E-cadherin IHC phenotype between the 2 antibodies (4A2C7 ≤ 10%/NCH38 ≥ 10%). Clinico-pathological correlation analyses found that stromal amount (inversely correlated with tumor cellularity) and tumor-infiltrating lymphocytes were less abundant in ILC with E-cadherin null/focal cases. In addition, CDH1 truncating mutations were associated with radiohistologic size discordance and were identified in multivariate survival analysis as an independent poor prognosis factor in terms of metastasis risk and breast cancer-related mortality. Overall, our study highlights the importance of the precise mutational status of CDH1 in the clinical, radiological, histologic, and phenotypic expression of lobular carcinomas. These findings should be taken into account in future attempts to improve diagnostic criteria or methods for ILC, as well as for clinicobiological studies dedicated to this tumor type.

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来源期刊
Modern Pathology
Modern Pathology 医学-病理学
CiteScore
14.30
自引率
2.70%
发文量
174
审稿时长
18 days
期刊介绍: Modern Pathology, an international journal under the ownership of The United States & Canadian Academy of Pathology (USCAP), serves as an authoritative platform for publishing top-tier clinical and translational research studies in pathology. Original manuscripts are the primary focus of Modern Pathology, complemented by impactful editorials, reviews, and practice guidelines covering all facets of precision diagnostics in human pathology. The journal's scope includes advancements in molecular diagnostics and genomic classifications of diseases, breakthroughs in immune-oncology, computational science, applied bioinformatics, and digital pathology.
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