Clinical Relevance of Tumour-Infiltrating Immune Cells in HER2-Negative Breast Cancer Treated with Neoadjuvant Therapy

Currently, therapy response cannot be accurately predicted in HER2-negative breast cancer (BC). Measuring stromal tumour-infiltrating lymphocytes (sTILs) and mediators of the tumour microenvironment and characterizing tumour-infiltrating immune cells (TIICs) may improve treatment response in the neo...

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Detalles Bibliográficos
Autores: Arqueros, Cristina|||0000-0003-1249-2324, Gallardo, Alberto|||0000-0002-2514-2027, Vidal, Silvia|||0000-0002-3909-6682, Osuna Gómez, Rubén|||0000-0003-2875-4405, Tibau Martorell, Ariadna|||0000-0003-0229-6987, Bell, Olga|||0009-0000-2858-6187, Ramon y Cajal, Teresa|||0000-0003-3490-3585, Lerma Puertas, Enrique|||0000-0001-7908-2747, Lobato-Delgado, Bárbara|||0000-0001-6218-5774, Salazar, Juliana|||0000-0002-3581-4499, Barnadas i Molins, Agustí|||0000-0002-0429-1349
Tipo de recurso: artículo
Fecha de publicación:2024
País:España
Institución:Universitat Autònoma de Barcelona
Repositorio:Dipòsit Digital de Documents de la UAB
Idioma:inglés
OAI Identifier:oai:ddd.uab.cat:291402
Acceso en línea:https://ddd.uab.cat/record/291402
https://dx.doi.org/urn:doi:10.3390/ijms25052627
Access Level:acceso abierto
Palabra clave:Breast cancer
Neoadjuvant chemotherapy
Stromal tumour-infiltrating lymphocytes
Tumour-infiltrating immune cells
Descripción
Sumario:Currently, therapy response cannot be accurately predicted in HER2-negative breast cancer (BC). Measuring stromal tumour-infiltrating lymphocytes (sTILs) and mediators of the tumour microenvironment and characterizing tumour-infiltrating immune cells (TIICs) may improve treatment response in the neoadjuvant setting. Tumour tissue and peripheral blood samples were retrospectively collected from 118 patients, and sTILs were evaluated. Circulating exosomes and myeloid-derived suppressor cells were determined by flow cytometry. TIICs markers (CD4, CD8, CD20, CD1a, and CD68) were assessed immunohistochemically. High sTILs were significantly associated with pathological complete response (pCR; p = 0.048) and event-free survival (EFS; p = 0.027). High-CD68 cells were significantly associated with pCR in triple-negative (TN, p = 0.027) and high-CD1a cells with EFS in luminal-B (p = 0.012) BC. Cluster analyses of TIICs revealed two groups of tumours (C1 and C2) that had different immune patterns and clinical outcomes. An immunoscore based on clinicopathological variables was developed to identify high risk (C1) or low-risk (C2) patients. Additionally, cluster analyses revealed two groups of tumours for both luminal-B and TNBC. Our findings support the association of sTILs with pCR and show an immunological component in a subset of patients with HER2-negative BC. Our immunoscore may be useful for future escalation or de-escalation treatments.