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循环肿瘤细胞的分子分析——生物学和生物标志物。

Molecular analysis of circulating tumour cells-biology and biomarkers.

机构信息

Clinical and Experimental Pharmacology Group, Cancer Research UK Manchester Institute, University of Manchester and Manchester Cancer Research Centre, 550 Wilmslow Road, Manchester M20 4BX, UK.

出版信息

Nat Rev Clin Oncol. 2014 Mar;11(3):129-44. doi: 10.1038/nrclinonc.2013.253. Epub 2014 Jan 21.

Abstract

Growing evidence for intratumour heterogeneity informs us that single-site biopsies fall short of revealing the complete genomic landscape of a tumour. With an expanding repertoire of targeted agents entering the clinic, screening tumours for genomic aberrations is increasingly important, as is interrogating the tumours for resistance mechanisms upon disease progression. Multiple biopsies separated spatially and temporally are impractical, uncomfortable for the patient and not without risk. Here, we describe how circulating tumour cells (CTCs), captured from a minimally invasive blood test-and readily amenable to serial sampling-have the potential to inform intratumour heterogeneity and tumour evolution, although it remains to be determined how useful this will be in the clinic. Technologies for detecting and isolating CTCs include the validated CellSearch(®) system, but other technologies are gaining prominence. We also discuss how recent CTC discoveries map to mechanisms of haematological spread, previously described in preclinical models, including evidence for epithelial-mesenchymal transition, collective cell migration and cells with tumour-initiating capacity within the circulation. Advances in single-cell molecular analysis are enhancing our ability to explore mechanisms of metastasis, and the combination of CTC and cell-free DNA assays are anticipated to provide invaluable blood-borne biomarkers for real-time patient monitoring and treatment stratification.

摘要

越来越多的肿瘤内异质性证据告诉我们,单点活检无法揭示肿瘤的完整基因组图谱。随着越来越多的靶向药物进入临床,筛选肿瘤的基因组异常变得越来越重要,在疾病进展时检测肿瘤的耐药机制也同样重要。多个空间和时间上分离的活检既不切实际,也让患者感到不适,而且并非没有风险。在这里,我们描述了如何从微创的血液检测中捕获循环肿瘤细胞(CTC),并且易于进行连续采样,这有可能为肿瘤内异质性和肿瘤进化提供信息,尽管尚不确定这在临床上有多大用处。检测和分离 CTC 的技术包括经过验证的 CellSearch(®)系统,但其他技术也越来越受到关注。我们还讨论了最近的 CTC 发现如何与临床前模型中先前描述的血液传播机制相吻合,包括上皮-间充质转化、集体细胞迁移和循环中具有肿瘤起始能力的细胞的证据。单细胞分子分析的进步增强了我们探索转移机制的能力,预计 CTC 和无细胞 DNA 检测的结合将为实时患者监测和治疗分层提供有价值的血液生物标志物。

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