HER2-positive breast cancer is defined by amplification or overexpression of the HER2/ERBB2 oncogene and accounts for about 15% of breast cancer cases. Somatic mutation of ERBB2 is an alternative mechanism, by which activation of HER2 signaling can occur. ERBB2 mutation has been associated with invasive lobular breast cancer (ILBC). This study investigates the frequency and phenotype of ILBC harboring mutated ERBB2. The ERBB2 mutation status was determined by next generation sequencing and/or pyrosequencing in n = 106 ILBCs, including n = 86 primary or locally recurrent tumors and n = 20 metastases from visceral organs, soft tissue, or skin.Immunohistochemical characteristics were determined using tissue microarrays. This series was enriched for ILBCs with pleomorphic histology and/or high-risk expression profiles (Oncotype DX, recurrence score RS > 25). Nearly all specimens were E-cadherin-negative (99%), estrogen receptor (ER)-positive (92%), and lacked ERBB2 overexpression (96%). ERBB2 mutations (p.V777L, p.L755S, p.S310F) were identified in 5/106 (5%) cases. ERBB2-mutated cases included 2/86 (2%) primary tumors and 3/20 (15%) metastases (P = 0.045). ERBB2-mutated cases were associated with loss of ER (2/7, 29%, P = 0.035) and histological grade 3 (4/34, 12%, P = 0.023), but not with solid growth (3/31, 10%, P = 0.148) or pleomorphic histology (2/27, 7%, P = 0.599). No ERBB2 mutation was detected in ILBCs with RS > 25 (0/22, 0%). In 10 patients with multiple matched specimens (n = 25), the ERBB2 mutational status was always concordant. In summary, a small subset of ILBCs harbors potentially actionable ERBB2 mutations. In ERBB2-mutated ILBCs, no association with pleomorphic histology was found.
K E Y W O R D SHER2/ERBB2 mutation, lobular breast cancer, Oncotype DX, recurrence score 1 | INTRODUCTION HER2-positive breast cancer is defined by amplification or overexpression of the HER2/ERBB2 oncogene and accounts for approximately 15% of breast cancer (BC) cases. 1-3 Somatic mutation of ERBB2 gene is a rare alternative mechanism, by which activation of HER2 signaling can occur. 4,5 Most ERBB2 mutations in BC affect the tyrosine kinase domain (amino acid residues 755-781) or the extracellular domain (amino acid residues 309-310). 4,5 These two different ERBB2 mutation types have different gain-of-function characteristics and enhance tyrosine kinase activity or dimerization, respectively. 4BCs harboring an ERBB2 mutations do not show overexpression of the mutant ERBB2 protein. 4 Except for rare instances, the mutated ERBB2 gene is not amplified. 4 Accordingly, conventional clinical HER2/ERBB2 assessment by immunohistochemistry and/or in situ hybridization fails to detect these cases. 4 Importantly, ERBB2 mutations are therapeutically relevant. In fact, recent clinical studies have shown that HER2/EGFR kinase inhibitors (lapatinib, neratinib) are highly effective in metastatic BCs harboring activating ERBB2 mutations. 6-8
