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早期乳腺癌中的微小残留病检测:综述

Minimal residue disease detection in early-stage breast cancer: a review.

作者信息

Zhang Yuan, Yuan Xiaoying

机构信息

College of Art and Science, Northeast Agricultural University, Changjiang Road No. 600, Harbin, 150030, China.

Shuwen Biotech Co., Ltd., Moganshan National High tech Zone, Building 3, No. 333, Changhong Middle Street, Deqing, China.

出版信息

Mol Biol Rep. 2025 Jan 7;52(1):106. doi: 10.1007/s11033-024-10198-0.

Abstract

Over the past five years, circulating tumor DNA (ctDNA) testing has emerged as a game-changer in cancer research, serving as a less invasive and highly sensitive method to monitor tumor dynamics. CtDNA testing has a wide range of potential applications in breast cancer (BC) management, including diagnosis, monitoring treatment responses, identifying resistance mutations, predicting prognosis, and detecting future relapses. In this review, we focus on the prognostic and predictive value of ctDNA testing for BC in both neoadjuvant and adjuvant settings. We also examine the rationale behind mainstream minimal residue disease (MRD) tracking methods and highlight key considerations for successful MRD testing. Clinical evidence has shown that ctDNA-based MRD testing can accurately detect molecular relapse 8-12 months before clinical relapse in early-stage BC. Compared to advanced-stage BC, detecting ctDNA in early-stage BC is more challenging and requires ultra-sensitive testing methods due to the low levels of ctDNA released into the bloodstream, particularly in post-surgical settings, after effective neoadjuvant chemotherapy, and in late adjuvant settings that require longer follow-up. Therefore, future efforts are needed to generate additional clinical evidence in these settings to support the clinical utility and widespread adoption of ctDNA-based MRD testing.

摘要

在过去五年中,循环肿瘤DNA(ctDNA)检测已成为癌症研究中的一项变革性技术,作为一种侵入性较小且高度灵敏的方法来监测肿瘤动态。CtDNA检测在乳腺癌(BC)管理中具有广泛的潜在应用,包括诊断、监测治疗反应、识别耐药突变、预测预后以及检测未来复发。在本综述中,我们聚焦于ctDNA检测在新辅助和辅助治疗背景下对BC的预后和预测价值。我们还探讨了主流微小残留病(MRD)追踪方法背后的原理,并强调成功进行MRD检测的关键考虑因素。临床证据表明,基于ctDNA的MRD检测可在早期BC临床复发前8 - 12个月准确检测到分子复发。与晚期BC相比,在早期BC中检测ctDNA更具挑战性,由于释放到血液中的ctDNA水平较低,特别是在术后、新辅助化疗有效后以及需要更长随访时间的晚期辅助治疗背景下,需要超灵敏的检测方法。因此,未来需要在这些背景下生成更多临床证据,以支持基于ctDNA的MRD检测的临床实用性和广泛应用。

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