Combination of automated high throughput platforms, flow cytometry, and hierarchical clustering to detect cell state

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Abstract

Background: This study examined whether hierarchical clustering could be used to detect cell states induced by treatment combinations that were generated through automation and high-throughput (HT) technology. Data-mining techniques were used to analyze the large experimental data sets to determine whether nonlinear, non-obvious responses could be extracted from the data. Methods: Unary, binary, and ternary combinations of pharmacological factors (examples of stimuli) were used to induce differentiation of HL-60 cells using a HT automated approach. Cell profiles were analyzed by incorporating hierarchical clustering methods on data collected by flow cytometry. Data-mining techniques were used to explore the combinatorial space for nonlinear, unexpected events. Additional small-scale, follow-up experiments were performed on cellular profiles of interest. Results: Multiple, distinct cellular profiles were detected using hierarchical clustering of expressed cell-surface antigens. Data-mining of this large, complex data set retrieved cases of both factor dominance and cooperativity, as well as atypical cellular profiles. Follow-up experiments found that treatment combinations producing "atypical cell types" made those cells more susceptible to apoptosis. Conclusions: Hierarchical clustering and other datamining techniques were applied to analyze large data sets from HT flow cytometry. From each sample, the data set was filtered and used to define discrete, usable states that were then related back to their original formulations. Analysis of resultant cell populations induced by a multitude of treatments identified unexpected phenotypes and nonlinear response profiles. © 2007 International Society for Analytical Cytology.

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Kitsos, C. M., Bhamidipati, P., Melnikova, I., Cash, E. P., McNulty, C., Furman, J., … Levinson, D. (2007). Combination of automated high throughput platforms, flow cytometry, and hierarchical clustering to detect cell state. Cytometry Part A, 71(1), 16–27. https://doi.org/10.1002/cyto.a.20353

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