Unraveling the clinicopathological and molecular changes induced by neoadjuvant chemotherapy and endocrine therapy in hormone receptor-positive/HER2-low and HER2-0 breast cancer

Author:

Schettini FrancescoORCID,Nucera Sabrina,Brasó-Maristany Fara,De Santo Irene,Pascual Tomás,Bergamino Milana,Galván Patricia,Conte Benedetta,Seguí Elia,García Fructuoso Isabel,Gómez Bravo Raquel,Rivera Pablo,Belén Rodríguez Ana,Martínez-Sáez Olga,Ganau Sergi,Sanfeliu Esther,González-Farre Blanca,Vidal Maria,Adamo Barbara,Cebrecos Isaac,Mension Eduard,Oses Gabriela,Jares Pedro,Vidal-Sicart Sergi,Mollà Meritxell,Muñoz Montserrat,Prat Aleix

Abstract

AbstractBackgroundThe characterization and comparison of gene expression (GE) and intrinsic subtypes (IS) changes induced by neoadjuvant chemotherapy (NACT) and endocrine therapy (NET) in hormone receptor-positive(HR+)/HER2-low vs. HR+/HER2-0 breast cancer (BC) has not been conducted so far. Most evidence on the association of HER2 status with pathologic responses and prognosis in HR+/HER2-negative BC is controversial and restricted to NACT-treated disease. Similarly, a temporal heterogeneity in HER2 status has been described only with NACT.MethodsWe retrospectively recruited a consecutive cohort of 186 patients with stage I-IIIB HR+/HER2-negative BC treated with neoadjuvant therapy (NAT). Available diagnostic biopsies and surgical samples were characterized for main pathological features, PAM50 intrinsic subtypes (IS) and risk-of-relapse (ROR)-P score, and GE. Associations with pathologic complete response (pCR), residual cancer burden (RCB)-0/I, event-free survival (EFS) and overall survival (OS) based on HER2 status were assessed. Pre/post pathologic/molecular changes were analyzed in matched samples.ResultsThe HER2-low (62.9%) and HER2-0 (37.1%) cohorts did not differ significantly in main baseline features, treatments administered, breast conserving surgery (BCS), pCR and RCB-0/I rates, EFS and OS. NAT induced, regardless of HER2 status, a significant reduction of ER/PgR and Ki67, a downregulation of PAM50 proliferation- and luminal-related genes/signatures, an upregulation of selected immune genes and a shift towards less aggressive IS and lower ROR-P. Moreover, 25% of HER2-0 changed to HER2-low and 34% HER2-low became HER2-0. HER2 shifts were significant after NACT (p<0.001), not NET (p=0.063), with consistentERBB2mRNA level dynamics. HER2 changes were not associated to EFS/OS.ConclusionsHER2 status changes after NAT in ∼1/4 of cases, mostly after NACT. Targeted adjuvant strategies should be investigated accordingly. Molecular downstaging with current chemo/endocrine agents and immunotherapy should not rely on HER2 immunohistochemical levels in HR+/HER2-negative BC. Instead, HER2-low-targeted approaches should be explored to pursue more effective and/or less toxic dimensional downstaging.HighlightsHormone receptor-positive (HR+)/HER2-low and HER2-0 breast cancer (BC) showed similar post-neoadjuvant surgical outcomes.Neoadjuvant therapy (NAT) induced a shift towards less aggressive subtypes and ROR-P classes regardless of HER2 status.All NAT strategies induced a downregulation of proliferation- and luminal biology-related genes, regardless of HER2 status.NAT induced changes in HER2 status, with a discordance rate of 34% and HER2-low showing higher instability than HER2-0.HER2 status at baseline, after surgery and its dynamics were not significantly associated to long-term outcomes.

Publisher

Cold Spring Harbor Laboratory

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