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Algorithm to identify circulating tumor cell clusters using in vivo flow cytometer

机译:使用体内流式细胞仪鉴定循环肿瘤细胞簇的算法

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Recent studies in oncology have addressed the importance of detecting circulating tumor cell clusters because circulating tumor cell clusters might survive and metastasize more easily than single circulating tumor cells. Signals with larger peak widths detected by in vivo flow cytometer (IVFC) have been used to identify cell clusters in previous studies. However, the accuracy of this criterion might be greatly degraded by variance in blood flow and the rolling behaviors of circulating tumor cells. Here, we propose a criterion and algorithm to distinguish cell clusters from single cells. In this work, we first used area-based and volume-based models for single fluorescent cells. Simulating each model, we analyzed the corresponding morphology of IVFC signals from cell clusters. According to the Rayleigh criterion, the valley between two adjacent peak signals from two distinguishable cells should be lower than 73.5% of the peak values. A novel signal processing algorithm for IVFC was developed based on this criterion. The results showed that cell clusters can be reliably identified using our proposed algorithm. Intravital imaging was also performed to further support our algorithm. With enhanced accuracy, IVFC is a powerful tool to study circulating cell clusters.
机译:肿瘤学方面的最新研究已经解决了检测循环肿瘤细胞簇的重要性,因为循环肿瘤细胞簇比单个循环肿瘤细胞更容易存活和转移。通过体内流式细胞仪(IVFC)检测到的具有较大峰宽的信号已用于鉴定先前研究中的细胞簇。但是,该标准的准确性可能会因血液流量的变化和循环肿瘤细胞的滚动行为而大大降低。在这里,我们提出了一种标准和算法来区分单个群集的细胞群集。在这项工作中,我们首先对单个荧光细胞使用了基于面积和基于体积的模型。模拟每个模型,我们分析了来自细胞簇的IVFC信号的相应形态。根据瑞利准则,来自两个可区分单元的两个相邻峰值信号之间的波谷应低于峰值的73.5%。基于此标准,开发了一种新的IVFC信号处理算法。结果表明,使用我们提出的算法可以可靠地识别细胞簇。还进行了玻璃体内成像,以进一步支持我们的算法。 IVFC具有增强的准确性,是研究循环细胞簇的强大工具。

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