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高速流式细胞术中的符合:模型与测量

Coincidence in high-speed flow cytometry: models and measurements.

作者信息

Keij J F, van Rotterdam A, Groenewegen A C, Stokdijk W, Visser J W

机构信息

Institute of Applied Radiobiology and Immunology TNO, Rijswijk, The Netherlands.

出版信息

Cytometry. 1991;12(5):398-404. doi: 10.1002/cyto.990120504.

Abstract

In flow cytometry, the coincident arrival of particles becomes a major problem when high sample rates are required. For the development of our high-speed photodamage flow cytometer (ZAPPER), it was of importance to understand the behavior of cells at flow rates of around 50,000-250,000 event/s. We developed and compared two models that describe the relation between the real cell rate and the detectable single cell rate. Both the Computer Simulation model and the Input/Output Device model show distinct optima for the cell rate. The models were compared to measurements performed on the ZAPPER-prototype. Fits of the two models to the experimental data were excellent for cycle times of 4 and 15 microseconds and acceptable for a 2 microseconds cycle time. A third model (Mercer WB, Rev. Sci. Instr. 37:1515-1521,1966) could be fitted to the experimental data, after the proportionality constant k was adapted to the experimental data. At a yield of detectable single cells of 70%, the maximum cell rates are 180,000, 100,000, and 40,000 cells/s for cycle times of 2, 4, and 15 microseconds, respectively. Based on these results we can now select an optimal cell rate for analysis and sorting based on criteria such as accepted cell loss. In addition, the advantages of reducing the cycle time can now be evaluated with respect to the costs of that modification.

摘要

在流式细胞术中,当需要高采样率时,粒子的同时到达就成为一个主要问题。对于我们高速光损伤流式细胞仪(ZAPPER)的开发而言,了解细胞在约50,000 - 250,000个事件/秒的流速下的行为非常重要。我们开发并比较了两个描述实际细胞速率与可检测单细胞速率之间关系的模型。计算机模拟模型和输入/输出设备模型都显示出细胞速率有明显的最优值。将这些模型与在ZAPPER原型上进行的测量结果进行了比较。对于4微秒和15微秒的循环时间,这两个模型与实验数据的拟合效果极佳,对于2微秒的循环时间,拟合效果尚可接受。在将比例常数k调整为与实验数据匹配后,第三个模型(Mercer WB,《科学仪器评论》37:1515 - 1521,1966)也能拟合实验数据。在可检测单细胞产率为70%时,对于2微秒、4微秒和15微秒的循环时间,最大细胞速率分别为180,000个细胞/秒、100,000个细胞/秒和40,000个细胞/秒。基于这些结果,我们现在可以根据诸如可接受的细胞损失等标准来选择用于分析和分选的最佳细胞速率。此外,现在可以根据修改成本来评估缩短循环时间的优势。

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