Abstract
HER2+ breast cancer (BC) is an aggressive subtype representing a genetically and biologically heterogeneous group of tumors resulting in variable prognosis and treatment response to HER2-targeted therapies according to estrogen (ER) and progesterone receptor (PR) expression. The relationship with androgen receptors (AR), a member of the steroid hormone’s family, is unwell known in BC. The present study aims to evaluate the prognostic impact of AR expression in HER2+ BC subtypes. A total of 695 BCs were selected and reviewed, AR, ER, PR and HER2 expression in tumor cells were examined by immunohistochemical method, and the SISH method was used in case of HER2 with equivocal immunohistochemical score (2+). A high prevalence of AR expression (91.5%) in BC HER+ was observed, with minimal differences between luminal and non-luminal tumor. According to steroid receptor expression, tumors were classified in four subgroups, including BC luminal and non-luminal HER2+ expressing or not AR. The luminal BC HER2 + AR+ was associated with lower histological grade, lower tumor size, higher PR expression and lower HER2 intensity of expression (2+). Also, the non-luminal tumors AR+ showed lower tumor size and lower prognostic stage but frequently higher grade and higher HER2 intensity of expression (3+). These findings should suggest a different progression of luminal and non-luminal tumors, both expressing AR, and allow us to speculate that the molecular mechanisms of AR, involved in the biology of BC HER2 + AR+, differ in relation to ER and PR expression. Moreover, AR expression may be a useful predictor of prognosis for overall survival (OS) in HER2+ BC subtypes. Our findings suggest that AR expression evaluation in clinical practice could be utilized in clinical oncology to establish different aggressiveness in BC HER2+ subtypes.
Highlights
Breast cancer (BC) is a heterogeneous disease enclosing several entities with different morphologic, prognostic and therapeutic features [1]
Tumors were grouped into four subtypes based on hormone receptors (ER, progesterone receptor (PR) and androgen receptors (AR)): Luminal B (LB) HER2 + AR+
AR is a steroid hormone receptor frequently expressed in BC, including the ERAR is a steroid hormone receptor frequently expressed in BC, including the ER-negnegative subtypes for which it could represent a complementary target for therapy, though ative subtypes for which it could represent a complementary target for therapy, though the clinical significance and functional role of AR has not been outlined in BC yet [40,41]
Summary
Breast cancer (BC) is a heterogeneous disease enclosing several entities with different morphologic, prognostic and therapeutic features [1]. Biomedicines 2022, 10, 164 according to histology and immunohistochemistry (i.e., ER, PR, HER2 overexpression, and/or HER2 gene amplification, and Ki67 proliferation index) [1,2]. Surrogate molecular classification of BC by means of immunohistochemistry defines specific subtypes, such as Luminal A (ER and PR positive, HER2 negative, low Ki67), Luminal B (ER positive, PR positive/negative, HER2 negative, high Ki67), Luminal B HER2+ (ER positive, PR positive/negative, HER2 positive, any Ki67), HER2+ non-luminal (ER-PR negative, HER2 positive, high Ki67), and triple negative (ER-PR-HER2 negative, high Ki67) [3,4]. BC immunohistochemistry surrogate classification has an actual utility in the management of BC patients having significant prognostic and predictive value [4]. HER2+ BCs include different histological subtypes: invasive BC no special type (IBCNST), lobular, micropapillary, apocrine, rarely mucinous [5].
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