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Gestational breast cancer: distinctive molecular and clinico-epidemiological features

流行病学 生物 乳腺癌 癌症 分子流行病学 病理 产科 生理学 妇科 遗传学 医学 基因 基因型
作者
Juan de la Haba-Rodríguez,Pablo Mínguez,Federico Rojo,Miguel Martín,Emilio Alba,Sònia Servitja,A. Prat,José Alejandro Pérez Fidalgo,Joaquín Gavilá,C Morales,A. Rodriguez-Lescure,Carmen Herrero,R Peña-Enriquez,Jesús Herránz,Cristina Hernándo,Abraham Hernández-Blanquisett,Silvia Guil‐Luna,María Teresa Martínez,S. Blanch,Rosalía Caballero,Natacha Martin,Marina Pollán,A. Guerrero-Zotano,Begoña Bermejo
出处
期刊:Journal of Mammary Gland Biology and Neoplasia [Springer Science+Business Media]
卷期号:29 (1)
标识
DOI:10.1007/s10911-024-09571-3
摘要

Gestational breast cancer (GBC), defined as breast cancer (BC) diagnosed during pregnancy or the first-year post-partum, accounts for 6-15% of BC cases in women aged 20-44 years. GBC has worse prognosis than non-GBC, but reasons behind are not clear. The GEICAM/2012-03 Study (Molecular Characterization of Gestational Breast Cancer) is a multicenter prospective/retrospective observational registry of patients diagnosed with GBC. From November 2014 to June 2015 seventy patients diagnosed with GBC were included in the study, 30 diagnosed during pregnancy and 40 after delivery. Our current study was aimed to explore differences in epidemiological, clinico-pathological and gene expression features of GBC tumors, from the GEICAM/2012-03 Study, compared to non-GBC tumors from patients of similar age (< 43 years) from six different GEICAM studies, used as non- GBC control population. As per the main objective, the study found multiple differences showing GBC tumors as a different biological entity. GBC showed a more aggressive biology, with higher Ki67 levels, higher incidence of breast and/or ovarian cancer family history, and germline deleterious BRCA1/2 mutations, and are enriched in basal-like intrinsic subtype. GBC patients showed a lower number of tumor infiltrating lymphocytes, while specific genetic signatures highlight differences in GBC´s distinctive transcriptome. Our study shows that GBC is potentially a clinically and molecularly different entity, with specific epidemiological, clinical, and histological features, as well as a distinctive altered immune state and genetic signature. Nevertheless, further studies are needed to better understand the biology of GBC and to identify new targets against which develop new, more effective, targeted therapies.

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