Liquid biopsy in breast cancer: Redefining precision medicine

Maria Luisa Schiavone , Rosa Scarpitta , Francesco Ravera , Sara Bleve , Carolina Reduzzi , Federico Di Cocco , Martina Dameri , Gabriele Zoppoli , Antonio Giuseppe Naccarato , Pier Vitale Nuzzo , Massimo Cristofanilli , Giuseppe Nicolò Fanelli , Cristian Scatena
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Abstract

Breast cancer (BC) is the most frequent cancer and the leading cause of cancer-related death among women worldwide. It represents a heterogeneous group of diseases with distinct morphological, immunophenotypic, and molecular profiles, which significantly impact clinical behavior and therapeutic response. Moreover, under treatment pressure, tumor cells may undergo molecular changes and phenotypic plasticity, leading to resistance and therapeutic failure. Although tissue biopsy remains the gold standard for diagnosis and molecular characterization, it has several limitations, including invasiveness, sampling bias, and the inability to dynamically capture tumor evolution over time. Hence, a non-invasive and repeatable approach capable of real-time monitoring is increasingly needed.
Liquid biopsy (LB), through the analysis of circulating tumor cells (CTCs) and circulating tumor DNA (ctDNA), has emerged as a powerful tool to complement tissue biopsy. It allows for longitudinal assessment of tumor burden, detection of minimal residual disease, and identification of molecular alterations relevant to targeted therapies. Despite promising results, the integration of LB into clinical practice is still limited by methodological heterogeneity, standardization gaps, and regulatory issues. Nonetheless, LB represents a key advancement toward precision oncology and may become essential in the personalized management of BC patients.
In this review, we explore the current applications, benefits, and technical limitations of LB in different BC settings. We provide a comprehensive overview of the biological and clinical significance of CTCs and ctDNA, emphasizing their diagnostic, prognostic, and predictive roles. Finally, we present an updated summary of ongoing clinical trials that incorporate LB for clinical decision-making.
乳腺癌液体活检:重新定义精准医学
乳腺癌(BC)是最常见的癌症,也是全世界妇女癌症相关死亡的主要原因。它代表了一组具有不同形态、免疫表型和分子特征的异质性疾病,这些疾病显著影响临床行为和治疗反应。此外,在治疗压力下,肿瘤细胞可能发生分子变化和表型可塑性,导致耐药性和治疗失败。尽管组织活检仍然是诊断和分子表征的金标准,但它有一些局限性,包括侵入性、采样偏差和无法动态捕捉肿瘤随时间的演变。因此,越来越需要一种能够实时监测的非侵入性和可重复的方法。液体活检(LB)通过对循环肿瘤细胞(CTCs)和循环肿瘤DNA (ctDNA)的分析,已成为组织活检的有力补充工具。它允许对肿瘤负荷进行纵向评估,检测最小残留疾病,并确定与靶向治疗相关的分子改变。尽管结果令人鼓舞,但将LB纳入临床实践仍然受到方法学异质性、标准化差距和监管问题的限制。尽管如此,LB代表了精确肿瘤学的关键进步,可能成为BC患者个性化管理的必要条件。在这篇综述中,我们探讨了LB在不同BC环境中的当前应用、优点和技术限制。我们全面概述了CTCs和ctDNA的生物学和临床意义,强调了它们的诊断、预后和预测作用。最后,我们提出了一份正在进行的临床试验的最新总结,这些试验将LB纳入临床决策。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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