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Cluster size distribution of cancer cells in blood using stopped-flow centrifugation along scale-matched gaps of a radially inclined rail

机译:使用沿径向倾斜轨道的比例匹配间隙的停流离心法,血液中癌细胞的簇大小分布

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摘要

There is increasing evidence that, in addition to their presence, the propensity of circulating tumour cells to form multi-cellular clusters bears significant information about both cellular resistance to chemotherapy and overall prognosis. We present a novel two-stage, stopped-flow, continuous centrifugal sedimentation strategy to measure the size distributions of events (defined here as cells or clusters thereof) in a blood sample. After off-chip removal of red blood cells, healthy white blood cells are sequestered by negative-immunocapture. The purified events are then resolved along a radially inclined rail featuring a series of gaps with increasing width, each connected to a designated outer collection bin. The isolation of candidate events independent of target-specific epitopes is successfully demonstrated for HL60 (EpCAM positive) and sk-mel28 (EpCAM negative) cells using identical protocols and reagents. The propensity to form clusters was quantified for a number of cell lines, showing a negligible, moderate or elevated tendency towards cluster formation. We show that the occupancy distribution of the collection bins closely correlates with the range of cluster sizes intrinsic to the specific cell line.
机译:越来越多的证据表明,除了循环肿瘤细胞的存在以外,形成多细胞簇的倾向还具有有关细胞对化疗的耐药性和总体预后的重要信息。我们提出了一种新颖的两阶段,停流,连续离心沉降策略,以测量血液样本中事件(在此定义为细胞或其簇)的大小分布。在芯片外去除红细胞后,阴性免疫捕获可以隔离健康的白细胞。然后,沿径向倾斜的轨道分解纯化的事件,该轨道具有一系列宽度逐渐增加的间隙,每个间隙都连接到指定的外部收集箱。 HL60(EpCAM阳性)和sk-mel28(EpCAM阴性)细胞已使用相同的方案和试剂成功地证明了独立于靶标特异性表位的候选事件的分离。对许多细胞系形成簇的倾向进行了定量,显示出簇形成的趋势可忽略不计,中等或升高。我们表明,收集箱的占用率分布与特定细胞系固有的簇大小范围密切相关。

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