Expression of amphiregulin and epidermal growth factor receptor in human breast cancer: analysis of autocriny and stromal–epithelial interactions

Amphiregulin (AR) and its receptor, epidermal growth factor receptor (EGFR), were evaluated by dual immunostaining in a series of 84 invasive ductal breast carcinoma specimens, 33 of which were from locally advanced inflammatory (T4d) cancer. Co‐expression of AR and EGFR was always found in non‐malignant breast tissues adjacent to tumours (24/24). Alternatively, expression of AR and EGFR was found in invasive epithelial tumour cells in 50% and 17.8% of specimens, respectively. In tumour stroma, 59.5% and 30.9% of specimens, respectively, were positively stained. By univariate analysis, AR and EGFR expression in invasive carcinomas was correlated with large tumour size, inflammatory carcinoma, node involvement, Bloom–Richardson (SBR) grade III, and absence of oestrogen receptor. EGFR expression in stromal cells was correlated with non‐inflammatory carcinoma. A putative autocrine loop with AR and EGFR expression in invasive carcinoma was detected in 14.3% of cases. Stromal expression of AR and EGFR expression in invasive tumour cells was detected in 11.9% of cases and related to poor prognostic parameters. By multivariate analysis, AR expression in invasive tumour was strongly related to inflammatory carcinoma ( p =0.005) and marginally related to SBR grade III ( p =0.07). EGFR expression in invasive tumour and stromal cells was correlated with absence of oestrogen receptor and non‐inflammatory carcinoma ( p =0.002 and p =0.015, respectively). Copyright © 2001 John Wiley & Sons, Ltd.