Biomarker Research Program Center, Houston Methodist Research Institute, TX, USA.
Department of Investigational Cancer Therapeutics, The University of Texas MD Anderson Cancer Center, Houston, TX, USA.
Mol Oncol. 2019 Sep;13(9):1913-1926. doi: 10.1002/1878-0261.12533. Epub 2019 Jun 19.
Triple-negative breast cancer (TNBC) liver metastasis is associated with poor prognosis and low patient survival. It occurs when tumor cells disseminate from primary tumors, circulate in blood/lymph [circulating tumor cells (CTCs)], and acquire distinct characteristics during disease progression toward the metastatic phenotype. The purpose of this study was to decipher the genomic/transcriptomic properties of TNBC liver metastasis and its recurrence for potential therapeutic targeting. We employed a negative depletion strategy to isolate and interrogate CTCs from the blood of patients with TNBC, and to establish sequential generations of CTC-derived xenografts (CDXs) through injection of patient CTCs in immunodeficient mice. The isolation and validation of CDX-derived cell populations [analyses of CTCs were paired with bone marrow-resident cells (BMRTCs) and liver tissue cells obtained from the same animal] were performed by multiparametric flow cytometry, immune phenotyping, and genomic sequencing of putative CTCs. Comprehensive characterization of gene expression arrays from sequentially generated CDX-derived cell populations, online gene expression arrays, and TCGA databases were employed to discover a CTC-driven, liver metastasis-associated TNBC signature. We discovered a distinct transcriptomic signature of TNBC patient-isolated CTCs from primary TNBCs, which was consistent throughout sequential CDX modeling. We established a novel TNBC liver metastasis-specific CDX model that selectively recapitulates CTC biology for four sequential generations of mice. The evaluation of online databases and CDX-derived populations revealed 597 genes specific to the TNBC liver metastasis signatures. Further investigation of the TNBC liver metastasis signature predicted 16 hub genes, 6 biomarkers with clinically available drugs, and 22 survival genes. The sequential interrogation of CDX-CTCs is an innovative liquid biopsy-based approach for the discovery of organ metastasis-specific signatures of CTCs. This represents the first step for mechanistic and analytical validation in their application as prognostic indicators and therapeutic targets. Targeting CTC drug candidate biomarkers along with combination therapy can improve the clinical outcome of TNBC patients in general and recurrence of liver metastasis in particular.
三阴性乳腺癌(TNBC)肝转移与预后不良和患者生存率低有关。当肿瘤细胞从原发性肿瘤扩散,在血液/淋巴中循环[循环肿瘤细胞(CTC)],并在向转移表型进展的过程中获得独特的特征时,就会发生这种情况。本研究的目的是破译 TNBC 肝转移及其复发的基因组/转录组特性,以寻找潜在的治疗靶点。我们采用负选择策略从 TNBC 患者的血液中分离和检测 CTC,并通过将患者的 CTC 注射到免疫缺陷小鼠中建立连续几代的 CTC 衍生异种移植物(CDX)。通过多参数流式细胞术、免疫表型分析和对假定 CTC 进行基因组测序,对 CDX 衍生细胞群的分离和验证[对 CTC 的分析与骨髓驻留细胞(BMRTC)和从同一动物获得的肝组织细胞进行配对]进行了分析。通过对连续产生的 CDX 衍生细胞群、在线基因表达阵列和 TCGA 数据库的基因表达阵列进行全面表征,发现了一个由 CTC 驱动的、与肝转移相关的 TNBC 特征。我们从原发性 TNBC 中发现了 TNBC 患者分离的 CTC 的独特转录组特征,在连续的 CDX 建模过程中始终保持一致。我们建立了一种新的 TNBC 肝转移特异性 CDX 模型,该模型可连续四代选择性地重现 CTC 生物学。对在线数据库和 CDX 衍生群体的评估揭示了与 TNBC 肝转移特征相关的 597 个特定基因。对 TNBC 肝转移特征的进一步研究预测了 16 个枢纽基因、6 个具有临床可用药物的生物标志物和 22 个生存基因。对 CDX-CTC 的连续检测是一种基于液体活检的创新方法,用于发现 CTC 器官转移特异性特征。这是将其作为预后指标和治疗靶点进行机制和分析验证的第一步。针对 CTC 药物候选生物标志物并结合联合治疗,可以改善一般 TNBC 患者的临床结局,特别是肝转移的复发。
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