Discordance of HER2-low Status between Breast Primary and Distant Metastases with Clinical-pathological Correlation

Author:

Yang Ellen1ORCID,D’Alfonso Timothy2,Morrow Monica1,Brogi Edi1ORCID,Wen Hannah1

Affiliation:

1. Memorial Sloan Kettering Cancer Center

2. Northwell Health

Abstract

Abstract

Introduction Breast cancer with HER2 immunohistochemistry (IHC) 1+ or 2+ with negative in situ hybridization (ISH) (HER2-low) can now be targeted by HER2 antibody drug conjugates. We set out to compare HER2 status between matched primary invasive breast carcinoma (IBC) and distant metastases (DM) with clinical-pathological correlation, with specific interest in HER2-low. Methods Biomarker studies and clinical-pathological features of primary IBC with matched DM diagnosed between 2021-2022 were retrospectively analyzed. HER2 status was assessed per 2023 ASCO/CAP guidelines for IHC (Ventana, 4B5) and ISH (IQFISH pharmDX, DAKO). Bilateral breast primaries were excluded. HER2 IHC 0 to 1+ were reassessed. Results 147 cases of primary IBC with matched DM were identified (Table 1). Biomarkers were performed on core biopsy (n=74) and resection (n=73). 126 cases (86%) were initially classified as “HER2 negative”; of these 67 (46%) were reclassified as HER2-low. Patients with HER2 positive primaries were younger (p=0.01) and had an increased incidence of micropapillary carcinoma (p=0.02). HER2-low primaries also had increased incidence of micropapillary carcinoma (p=0.02) and estrogen receptor (ER) positivity (p=0.02) comparing to HER2 0. 169 matched DM cases excluding bone metastasis were identified (range of 1-7 metastases per IBC). The most common sites of metastases were liver (50/169, 30%), lung (36/169; 21%), distant lymph node (26/169, 15%). 138 DM cases (82%) were previously classified as “HER2 negative”, and 62 (37%) were reclassified as HER2-low. Like HER2-low primaries, HER2-low metastases were frequently ER positive (52/62; 84%) (p=0.02). Brain metastases were more frequently HER2 positive (5/32; 16%) (p=0.04). Comparing HER2 status in matched primaries and DM, HER2 status was discordant in 62 cases (37%). Most changes occurred from HER2-low to HER2 0 (33/169, 20 %), HER2 0 to HER2-low (17/169, 10%), and HER2-low to positive (10/169, 6%). All HER2-low to HER2 0 changes were HER2 1+ to 0. In 30 patients with multiple DM sites (47 cases), HER2 status among different DM samples was discordant in 16 patients (53%), mostly from HER2-low to HER2 0 (16/47, 34 %). Conclusion Significant proportion of previous “HER2 negative” primaries and DM cases are reclassified as HER2-low. Discordant HER2 status between IBC primary and metastasis and between different DM sites demonstrated tumor heterogeneity and highlights the need for HER2 retesting in distant metastasis.

Publisher

Research Square Platform LLC

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