Dual HER2 inhibition: mechanisms of synergy, patient selection, and resistance

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Publicated to:Nature Reviews Clinical Oncology. 21 (11): 818-832 - 2024-09-13 21(11), DOI: 10.1038/s41571-024-00939-2

Authors: Waks, AG; Tarantino, P; Tolaney, SM; Martínez-Sáez, O; Braso-Maristany, F; Pascual, T; Prat, A; Cortés, J

Affiliations

Dana Farber Brigham Canc Ctr, Breast Oncol Program, Boston, MA USA - Author

Dana Farber Canc Inst, Med Oncol, Boston, MA USA - Author

Harvard Med Sch, Boston, MA USA - Author

Hosp Beata Maria Ana, IOB Madrid, Madrid, Spain - Author

Hosp Clin Barcelona, Canc Inst, Barcelona, Spain - Author

Inst Invest Biomed August Pi & Sunyer IDIBAPS, Barcelona, Spain - Author

IOB QuironSalud, Breast Canc Unit, Barcelona, Spain - Author

QuironSalud Grp, Int Breast Canc Ctr IBCC, Pangaea Oncol, Barcelona, Spain - Author

Reveal Genom, Barcelona, Spain - Author

SOLTI Canc Res Grp, Barcelona, Spain - Author

Univ Barcelona, Dept Med, Barcelona, Spain - Author

Univ Europea Madrid, Fac Biomed & Hlth Sci, Dept Med, Madrid, Spain - Author

Univ Milan, Dept Oncol & Hemato Oncol, Milan, Italy - Author

Abstract

HER2-targeted therapies for patients with HER2+ breast cancer are rapidly evolving, offering a range of more complex and personalized treatment options. Currently, an array of anti-HER2 monoclonal antibodies, tyrosine kinase inhibitors and antibody-drug conjugates are administered, sometimes alongside chemotherapy or endocrine therapy, both in curative and palliative contexts. However, the heterogeneous nature of HER2+ breast cancer demands a deeper understanding of disease biology and its role in responsiveness to novel HER2-targeted agents, as well as non-HER2-targeted therapies, in order to optimize patient outcomes. In this Review, we revisit the mechanisms of action of HER2-targeted agents, examine the evidence supporting the use of dual HER2 blockade in patients with HER2-amplified tumours, and explore the role of biomarkers in guiding future treatment strategies. We also discuss potential implications for the future treatment of patients with HER2+ breast cancer. Patients with HER2+ breast cancer often respond to trastuzumab, although acquired resistance is common and can involve a range of mechanisms. reflecting the highly heterogeneous biology of this breast cancer subtype. In this Review, the authors describe the role of dual HER2 blockade, involving the co-administration of two HER2-targeted therapies (including monoclonal antibodies, tyrosine kinase inhibitors and antibody-drug conjugates) in patients with HER2+ breast cancer. HER2-targeted therapies function by blocking activation of the oncogenic tyrosine kinase signalling pathways downstream of HER2 and inducing immune-mediated cell death.Dual HER2 inhibition can overcome resistance to single-agent blockade through several mechanisms, including more potent inhibition of downstream signalling pathways, overcoming limited HER2 binding, and augmenting HER2 receptor downregulation and degradation.Regimens including trastuzumab plus pertuzumab improve pathological complete response and long-term event rates in patients with stage II-III HER2+ breast cancer receiving neoadjuvant or adjuvant therapy, respectively, compared with trastuzumab monotherapy.Compared with single-agent HER2 inhibition, dual inhibition improves the outcomes of patients with HER2+ metastatic breast cancer in both the first-line and treatment-refractory settings, thus underscoring the importance of oncogenic HER2 signalling throughout the course of disease.HER2+ breast cancer is a biologically heterogeneous disease. Biomarkers including level of HER2 expression, luminal biology, tumour cell proliferation and tumour immune infiltration all merit further investigation as possible methods of guiding the selection of HER2-targeted therapies.

Keywords

Anti-her2 monoclonal-antibodyAntibody drug conjugateAntineoplastic agentAntineoplastic combined chemotherapy protocolsBiological markerBiomarkers, tumorBreast neoplasmsBreast tumorDrug combinationDrug potentiationDrug resistanceDrug resistance, neoplasmDrug synergismDrug therapyEpidermal growth factor receptor 2Erbb2 protein, humanFemaleFinal analysiFree chemotherapy regimensGeneticsGrowth-factor receptorHer2-positive breast-cancerHumanHuman epidermal growth factor receptor 2 positive breast cancerHumansMetabolismMolecular targeted therapyMolecularly targeted therapyMonoclonal antibodyNeoplastic cell transformationOpen-labelPathological complete responsePathologyPatient selectionPersonalized medicinePertuzumab plus trastuzumabPhase-iiProceduresProtein kinase inhibitorProtein kinase inhibitorsReceptor, erbb-2ReviewTherapyTumor markerTumor-infiltrating lymphocytes

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The work has been published in the journal Nature Reviews Clinical Oncology due to its progression and the good impact it has achieved in recent years, according to the agency WoS (JCR), it has become a reference in its field. In the year of publication of the work, 2024 there are still no calculated indicators, but in 2023, it was in position 2/322, thus managing to position itself as a Q1 (Primer Cuartil), in the category Oncology. Notably, the journal is positioned above the 90th percentile.

Independientemente del impacto esperado determinado por el canal de difusión, es importante destacar el impacto real observado de la propia aportación.

Según las diferentes agencias de indexación, el número de citas acumuladas por esta publicación hasta la fecha 2025-06-30:

Scopus: 6

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This work has been carried out with international collaboration, specifically with researchers from: Italy; United States of America.

the author responsible for correspondence tasks has been Prat Aparicio, Aleix.

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