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治疗反应和肿瘤演变:从转移性乳腺癌患者一系列延长的多分析物液体活检中得到的经验。

Treatment response and tumor evolution: lessons from an extended series of multianalyte liquid biopsies in a metastatic breast cancer patient.

机构信息

Convergent Science Institute in Cancer, Michelson Center for Convergent Bioscience, University of Southern California, Los Angeles, California 90089, USA.

The Scripps Research Institute, La Jolla, California 92037, USA.

出版信息

Cold Spring Harb Mol Case Stud. 2020 Dec 17;6(6). doi: 10.1101/mcs.a005819. Print 2020 Dec.

Abstract

Currently, clinical characterization of metastatic breast cancer is based on tissue samples taken at time of diagnosis. However, tissue biopsies are invasive and tumors are continuously evolving, which indicates the need for minimally invasive longitudinal assessment of the tumor. Blood-based liquid biopsies provide minimal invasive means for serial sampling over the course of treatment and the opportunity to adjust therapies based on molecular markers. Here, we aim to identify cellular changes that occur in breast cancer over the lifespan of an affected patient through single-cell proteomic and genomic analysis of longitudinally sampled solid and liquid biopsies. Three solid and 17 liquid biopsies from peripheral blood of an ER/HER2 metastatic breast cancer patient collected over 4 years and eight treatment regimens were analyzed for morphology, protein expression, copy-number alterations, and single-nucleotide variations. Analysis of 563 single morphometrically similar circulating tumor cells (CTCs) and 13 cell-free DNA (cfDNA) samples along with biopsies of the primary and metastatic tumor revealed progressive genomic evolution away from the primary tumor profiles, along with changes in ER expression and the appearance of resistance mutations. Both the abundance and the genomic alterations of CTCs and cfDNA were highly correlated and consistent with genomic alterations in the tissue samples. We demonstrate that genomic evolution and acquisition of drug resistance can be detected in real time and at single-cell resolution through liquid biopsy analytes and highlight the utility of liquid biopsies to guide treatment decisions.

摘要

目前,转移性乳腺癌的临床特征基于诊断时采集的组织样本。然而,组织活检具有侵入性,且肿瘤不断进化,这表明需要对肿瘤进行微创的纵向评估。基于血液的液体活检为治疗过程中的连续采样提供了微创手段,并为基于分子标志物调整治疗方法提供了机会。在这里,我们旨在通过对纵向采样的固体和液体活检进行单细胞蛋白质组学和基因组分析,来识别乳腺癌在受影响患者一生中发生的细胞变化。对一名 ER/HER2 转移性乳腺癌患者的 3 份实体和 17 份外周血液体活检进行了 4 年 8 个治疗方案的分析,用于形态学、蛋白表达、拷贝数改变和单核苷酸变异分析。对 563 个形态相似的循环肿瘤细胞(CTC)和 13 个无细胞 DNA(cfDNA)样本进行分析,以及原发和转移性肿瘤的活检,结果显示肿瘤基因组从原发肿瘤图谱中逐渐进化,同时 ER 表达发生变化,出现耐药突变。CTC 和 cfDNA 的丰度和基因组改变都与组织样本的基因组改变高度相关且一致。我们证明,通过液体活检分析物可以实时、单细胞分辨率检测到基因组进化和获得耐药性,并强调液体活检在指导治疗决策方面的实用性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e5d2/7784493/43f89aaaf4cf/MCS005819Wel_F1.jpg

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