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采血试管类型和处理时间对使用高清单细胞分析技术检测循环肿瘤细胞的计数和高内涵特征的影响。

Effect of Blood Collection Tube Type and Time to Processing on the Enumeration and High-Content Characterization of Circulating Tumor Cells Using the High-Definition Single-Cell Assay.

出版信息

Arch Pathol Lab Med. 2018 Feb;142(2):198-207. doi: 10.5858/arpa.2016-0483-OA. Epub 2017 Nov 16.

Abstract

CONTEXT

  • As circulating tumor cell (CTC) assays gain clinical relevance, it is essential to address preanalytic variability and to develop standard operating procedures for sample handling in order to successfully implement genomically informed, precision health care.

OBJECTIVE

  • To evaluate the effects of blood collection tube (BCT) type and time-to-assay (TTA) on the enumeration and high-content characterization of CTCs by using the high-definition single-cell assay (HD-SCA).

DESIGN

  • Blood samples of patients with early- and advanced-stage breast cancer were collected into cell-free DNA (CfDNA), EDTA, acid-citrate-dextrose solution, and heparin BCTs. Time-to-assay was evaluated at 24 and 72 hours, representing the fastest possible and more routine domestic shipping intervals, respectively.

RESULTS

  • We detected the highest CTC levels and the lowest levels of negative events in CfDNA BCT at 24 hours. At 72 hours in this BCT, all CTC subpopulations were decreased with the larger effect observed in high-definition CTCs and cytokeratin-positive cells smaller than white blood cells. Overall cell retention was also optimal in CfDNA BCT at 24 hours. Whole-genome copy number variation profiles were generated from single cells isolated from all BCT types and TTAs. Cells from CfDNA BCT at 24-hour TTA exhibited the least noise.

CONCLUSIONS

  • Circulating tumor cells can be identified and characterized under a variety of collection, handling, and processing conditions, but the highest quality can be achieved with optimized conditions. We quantified performance differences of the HD-SCA for specific preanalytic variables that may be used as a guide to develop best practices for implementation into patient care and/or research biorepository processes.
摘要

背景

随着循环肿瘤细胞(CTC)检测在临床上的相关性不断增强,解决分析前的变异性问题并制定样本处理的标准操作规程对于成功实施基于基因组信息的精准医疗至关重要。

目的

通过使用高通量单细胞分析(HD-SCA)评估血液采集管(BCT)类型和检测时间(TTA)对 CTC 计数和高内涵特征分析的影响。

设计

采集早期和晚期乳腺癌患者的无细胞 DNA(cfDNA)、EDTA、柠檬酸葡萄糖溶液和肝素 BCT 样本。分别在 24 小时和 72 小时评估 TTA,这分别代表最快和更常规的国内运输间隔。

结果

我们在 24 小时时在 cfDNA BCT 中检测到最高的 CTC 水平和最低的阴性事件水平。在 72 小时时,cfDNA BCT 中所有 CTC 亚群均减少,高内涵 CTC 和白细胞小的细胞角蛋白阳性细胞减少更为明显。在 24 小时时,cfDNA BCT 的整体细胞保留也最佳。从所有 BCT 类型和 TTA 分离的单细胞生成了全基因组拷贝数变异图谱。在 24 小时 TTA 时,cfDNA BCT 中的细胞噪声最小。

结论

可以在各种采集、处理和处理条件下识别和分析循环肿瘤细胞,但通过优化条件可以获得最佳质量。我们量化了 HD-SCA 在特定分析前变量方面的性能差异,这些差异可以作为指导,为患者护理和/或研究生物库流程制定最佳实践提供依据。

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