Sánchez-Espinosa Alberto, García-Rodríguez José, Alonso-Aguirre Virginia, Acosta-Ortega Jesús María, Conesa-Zamora Pablo, García-Solano José, Luengo-Gil Ginés
Group of Molecular Pathology and Pharmacogenetics, Pathology Department, Instituto Murciano de Investigación Biosanitaria (IMIB), Hospital Universitario Santa Lucía, 30202 Cartagena, Spain.
Health Sciences Faculty, Universidad Católica de Murcia (UCAM), 30107 Guadalupe, Spain.
Int J Mol Sci. 2025 Mar 27;26(7):3076. doi: 10.3390/ijms26073076.
BACKGROUND/OBJECTIVES: Breast cancer is the most prevalent cancer in adult women. Currently, new therapies and protein determinations with prognostic value are under development. Fascin (encoded by the gene) is an actin-binding protein that is critical for the development of cytoplasmic projections that are essential for tumor invasion. DNA topoisomerase 2-alpha () is a nuclear protein crucial for ATP-dependent breakage, passage, and rejoining of double-stranded DNA and cell division. Both proteins are associated with higher proliferation rates and worse prognosis in breast cancer and together can provide comprehensive information on prognosis and treatment response.
We simultaneously assessed fascin expression and TOP2A/CEP17 DNA copy number ratios in various histological and molecular subtypes. Additionally, these markers were analyzed along with previously established diagnostic markers and other relevant clinical data.
Our series included 265 patients, four of whom were male, and all of which were diagnosed with breast carcinoma. Of the 265 patients initially included, sufficient material for analysis was available for 175 cases, as some samples were excluded because of insufficient tissue quantity, poor preservation, or lack of hybridization in certain assays. Immunohistochemical (IHC) expression of fascin, both in its aggregated form and by category, showed no association with the TOP2A gene alteration ratio. Fascin expression was significantly associated with histological subtype ( < 0.001), molecular subtype ( < 0.001), hormone receptor (HR) ( < 0.001), BCL2 ( = 0.003), Ki67 ( = 0.002), and histological grade ( < 0.001). TOP2A was significantly associated with molecular subtype ( = 0.041), Ki67 ( = 0.048), and histological grade ( = 0.033). In our study, molecular subtype ( = 0.037) emerged as an independent variable for the complete histological response to neoadjuvant treatment. Multivariate analysis linked pathological stage ( = 0.002) and estrogen receptor (ER) expression ( = 0.004) to overall survival (OS) and disease-free survival (DFS).
No statistical relationship was evident between fascin expression (IHC) and the TOP2A copy ratio. The results of this study suggested that the mechanisms of increased cell proliferation associated with alterations in fascin and TOP2A are independent.
背景/目的:乳腺癌是成年女性中最常见的癌症。目前,具有预后价值的新疗法和蛋白质测定方法正在研发中。Fascin(由该基因编码)是一种肌动蛋白结合蛋白,对肿瘤侵袭所必需的细胞质突起的形成至关重要。DNA拓扑异构酶2-α()是一种核蛋白,对双链DNA的ATP依赖性断裂、通过和重新连接以及细胞分裂至关重要。这两种蛋白都与乳腺癌中较高的增殖率和较差的预后相关,并且共同可以提供关于预后和治疗反应的全面信息。
我们同时评估了各种组织学和分子亚型中Fascin的表达以及TOP2A/CEP17 DNA拷贝数比率。此外,还将这些标志物与先前建立的诊断标志物和其他相关临床数据一起进行了分析。
我们的系列研究包括265例患者,其中4例为男性,所有患者均被诊断为乳腺癌。在最初纳入的265例患者中,有175例有足够的分析材料,因为一些样本由于组织量不足、保存不佳或某些检测中缺乏杂交而被排除。Fascin的免疫组织化学(IHC)表达,无论是其聚集形式还是按类别,均与TOP2A基因改变比率无关。Fascin表达与组织学亚型(<0.001)、分子亚型(<0.001)、激素受体(HR)(<0.001)、BCL2(=0.003)、Ki67(=0.002)和组织学分级(<0.001)显著相关。TOP2A与分子亚型(=0.041)、Ki67(=0.048)和组织学分级(=0.033)显著相关。在我们的研究中,分子亚型(=0.037)成为新辅助治疗完全组织学反应的独立变量。多变量分析将病理分期(=0.002)和雌激素受体(ER)表达(=0.004)与总生存期(OS)和无病生存期(DFS)相关联。
Fascin表达(IHC)与TOP2A拷贝比率之间无明显统计学关系。本研究结果表明,与Fascin和TOP2A改变相关的细胞增殖增加机制是独立的。
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