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Heterogeneity of PIK3CA mutational status at the single cell level in circulating tumor cells from metastatic breast cancer patients

机译:转移性乳腺癌患者循环肿瘤细胞中单细胞水平上PIK3CA突变状态的异质性

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摘要

Circulating Tumor Cells (CTCs) represent a “liquid biopsy of the tumor” which might allow real‐time monitoring of cancer biology and therapies in individual patients. CTCs are extremely rare in the blood stream and their analysis is technically challenging.The CellSearch® system provides the enumeration of CTCs with prognostic significance in patients with metastatic breast cancer (mBC), but it does not allow their molecular characterization, which might be useful to identify therapeutically relevant targets for individualized treatment. Combining the CellSearch® and DEPArray™ technologies allows the recovery of single CTCs as a pure sample for molecular analysis.The purpose of the study was to investigate the heterogeneity of PIK3CA mutational status within single CTCs isolated from individual mBC patients.CTCs were enriched and enumerated by CellSearch® in blood samples collected from 39 mBC patients. In 20 out of 39 patients enriched samples with ≥5 CTCs were sorted using DEParray™ to isolate single CTCs or pools of CTCs to be submitted to Whole Genome Amplification (WGA) before sequencing analysis. In 18 out of 20 patients, it was possible to perform PIK3CA sequencing on exons 9 and 20.Twelve subjects were wild type (wt) for the PIK3CA gene. PIK3CA status could also be assessed in pools of CTCs in seven of these patients, with consistent wt status found. Six patients (33%) had a PIK3CA mutation identified. In 2 of the six patients, molecular heterogeneity was detected when mutational analysis was performed on more than one single CTC, including one patient with loss of heterozygosity on both single and pooled CTCs, and one patient with three different PIK3CA variants on single CTCs but PIK3CA wt status on pooled CTC samples. In six out of the 18 cases PIK3CA status was also evaluable on a primary tumor sample. In one of the six cases a discordance in PIK3CA status between the primary (wild‐type) and the matched CTC (exon 20 mutation) was observed.This study demonstrates the feasibility of a non‐invasive approach based on the liquid biopsy in mBC patients.Moreover, our data suggest the importance of characterizing CTCs at the single cell level in order to investigate the molecular heterogeneity within cells from the same patient.
机译:循环肿瘤细胞(CTC)代表“肿瘤的液体活检”,这可能允许实时监测单个患者的癌症生物学和疗法。 CTC在血液中极为罕见,其分析在技术上具有挑战性。CellSearch®系统提供了对CTC的计数,对转移性乳腺癌(mBC)患者具有预后意义,但它不允许对其分子进行表征,这可能是有用的确定个体化治疗的治疗相关靶标。结合CellSearch®和DEPArray™技术,可以回收单个CTC作为分子分析的纯样品。本研究的目的是研究从单个mBC患者中分离出的单个CTC中PIK3CA突变状态的异质性。通过CellSearch®在39例mBC患者的血液样本中进行检测。在39例患者中,有20例使用DEParray™分选了≥5个CTC的富集样品,以分离单个CTC或CTC库,在进行测序分析之前先进行全基因组扩增(WGA)。在20名患者中的18名患者中,有可能对9号和20号外显子进行PIK3CA测序。十二名受试者是PIK3CA基因的野生型(wt)。也可以在其中7名患者的CTC池中评估PIK3CA状态,并发现一致的wt状态。确定了六名患者(33%)具有PIK3CA突变。在六名患者中的两名患者中,当对一个以上的单个CTC进行突变分析时,发现了分子异质性,包括一名患者在单个CTC和合并的CTC上均失去杂合性,以及一名患者在单个CTC上具有三种不同的PIK3CA变异体,但PIK3CA合并的四氯化碳样品的wt状态。在18例病例中,有6例在原发肿瘤样本中也可以评估PIK3CA的状态。在六例病例之一中,观察到原发性(野生型)和匹配的CTC(外显子20突变)之间PIK3CA状态不一致。本研究证明了基于液体活检的非侵入性方法在mBC患者中的可行性此外,我们的数据表明在单细胞水平上表征CTC的重要性,以研究同一患者细胞内的分子异质性。

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