HER2阴性原发性肿瘤的HER2低表达转移灶:一项单机构对淋巴结阳性乳腺癌瘤间和淋巴结内异质性的分析
HER2-low metastases of HER2-negative primary tumors: a single institution analysis of intertumoral and internodal heterogeneity in node-positive breast cancer.
作者信息
Pellas Ulrika, Bauer Annette, Baroš Ilija Vladimir, Fattorini Caterina, Tot Tibor
机构信息
Unit for Research and Higher Education, Centre for Clinical Research Dalarna, Uppsala University, Region Dalarna, Falun, Sweden.
Pathology and Cytology Dalarna, County Hospital Falun, Region Dalarna, Falun, Sweden.
出版信息
Front Oncol. 2023 Jul 7;13:1167567. doi: 10.3389/fonc.2023.1167567. eCollection 2023.
OBJECTIVE
HER2 status in breast cancer is an essential parameter in individual therapeutic decision-making and is routinely assessed in primary tumors in accordance with international recommendations. Reports of HER2 heterogeneity raise the question of basing treatment decisions on HER2 status in metastases, if present. We investigated the degree and clinical implications of HER2 heterogeneity in lymph node-positive breast cancer. Because of recent recognition of therapeutic opportunities in this group of tumors, we especially focused on cases involving low-level HER2 expression.
METHODS
The HER2 status of primary tumors and of corresponding lymph node metastases was determined in archived material at the protein and gene levels using the gene- protein assay and interpreted in accordance with 2018 ASCO/CAP criteria. HER2-low status was defined as protein expression levels 1+ or 2+ with negative amplification status.
RESULTS
We analyzed a series of 43 cases of primary infiltrating breast cancer, each with at least two axillary nodes harboring macrometastases (>2 mm), in total 206 such nodes. In 7% of cases, we detected intertumoral HER2 heterogeneity. Three of nine HER2-positive primary tumors were associated with HER2-negative metastases. No cases with HER2-negative primary tumors had HER2-positive metastases, but 55% (6/11) of HER2 0 primary tumors had HER2 1+ and/or 2+ metastases, and 19% (3/16) HER2 1+ cases had exclusively HER2 0 metastases. All metastases in HER2 2+ cases showed HER2-low protein expression levels. Internodal HER2 heterogeneity at low protein expression levels (presence of HER2 0, HER2 1+, and/or HER2 2+ metastatic deposits within the same axilla) was seen in 40% (17/43) of cases. We found no statistically significant association between HER2 heterogeneity and other tumor-related parameters. Survival data indicated worse outcomes in the HER2-low group compared with the rest of the cohort.
CONCLUSION
Our results indicate a substantial instability of HER2 protein expression, leading to considerable intertumoral and internodal HER2 heterogeneity in lymph node-positive breast carcinomas. This heterogeneity is particularly relevant in HER2-low tumors in which the corrective effects of HER2 gene copy number analysis definitionally is absent. Our findings suggest that determining HER2 status in metastatic lymph nodes may generate relevant information for therapeutic decision-making.
目的
HER2在乳腺癌中的状态是个体治疗决策的重要参数,并且根据国际建议在原发性肿瘤中进行常规评估。关于HER2异质性的报道提出了一个问题,即如果存在转移灶,是否应根据转移灶中的HER2状态来做出治疗决策。我们研究了HER2异质性在淋巴结阳性乳腺癌中的程度及其临床意义。由于最近认识到这组肿瘤的治疗机会,我们特别关注了HER2低表达的病例。
方法
使用基因-蛋白质检测法在存档材料中从蛋白质和基因水平确定原发性肿瘤及其相应淋巴结转移灶的HER2状态,并根据2018年美国临床肿瘤学会/美国病理学家学会(ASCO/CAP)标准进行解读。HER2低状态定义为蛋白质表达水平为1+或2+且扩增状态为阴性。
结果
我们分析了一系列43例原发性浸润性乳腺癌病例,每例至少有两个腋窝淋巴结存在大转移灶(>2 mm),共计206个此类淋巴结。在7%的病例中,我们检测到肿瘤间HER2异质性。9例HER2阳性原发性肿瘤中有3例与HER2阴性转移灶相关。没有HER2阴性原发性肿瘤出现HER2阳性转移灶,但55%(6/11)的HER2 0原发性肿瘤有HER2 1+和/或2+转移灶,19%(3/16)的HER2 1+病例仅有HER2 0转移灶。HER2 2+病例中的所有转移灶均显示HER2低蛋白表达水平。在40%(17/43)的病例中观察到低蛋白表达水平的淋巴结内HER2异质性(同一腋窝内存在HER2 0、HER2 1+和/或HER2 2+转移沉积物)。我们发现HER2异质性与其他肿瘤相关参数之间无统计学显著关联。生存数据表明,HER2低表达组的预后比其余队列更差。
结论
我们的结果表明HER2蛋白表达存在显著不稳定性,导致淋巴结阳性乳腺癌中存在相当程度的肿瘤间和淋巴结内HER2异质性。这种异质性在HER2低表达肿瘤中尤为相关,因为在这些肿瘤中HER2基因拷贝数分析的校正作用从定义上说是不存在的。我们的研究结果表明,确定转移性淋巴结中的HER2状态可能为治疗决策提供相关信息。
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