README.md
In cytolab/RAPID: Risk Assessment Population Identification
RAPID: Risk Assessment Population and Identification
RAPID pre-print available via bioRxiv:
https://www.biorxiv.org/content/10.1101/632208v3
Risk Assessment Population IDentification (RAPID) is an unsupervised, machine learning algorithm that identifies single cell phenotypes and assesses clinical risk stratification as a continuous variable.
This repository contains the code for the computational workflow as well as example data from 2018 Davis et al. (https://www.ncbi.nlm.nih.gov/pubmed/29505032)
Figure 1:
RAPID identifies single cell phenotypes and assesses clinical risk stratification as a continuous variable.
(a) Graphic of tumor processing and computational workflow. (b) Glioblastoma cells were identified from 28 patients and computationally pooled for a t-SNE analysis. Cell subsets were automatically identified by FlowSOM and were systematically assessed for association with patient overall or progression-free survival. 43 glioblastoma cell subsets were identified and were color-coded based on hazard ratio of death and p-values (HR>1, red; HR<1, blue) Cell density, FlowSOM cluster, and cluster significance are depicted on t-SNE plots.
cytolab/RAPID documentation built on May 9, 2022, 2:55 p.m.
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RAPID: Risk Assessment Population and Identification
RAPID pre-print available via bioRxiv:
https://www.biorxiv.org/content/10.1101/632208v3
Risk Assessment Population IDentification (RAPID) is an unsupervised, machine learning algorithm that identifies single cell phenotypes and assesses clinical risk stratification as a continuous variable.
This repository contains the code for the computational workflow as well as example data from 2018 Davis et al. (https://www.ncbi.nlm.nih.gov/pubmed/29505032)
Figure 1:
RAPID identifies single cell phenotypes and assesses clinical risk stratification as a continuous variable. (a) Graphic of tumor processing and computational workflow. (b) Glioblastoma cells were identified from 28 patients and computationally pooled for a t-SNE analysis. Cell subsets were automatically identified by FlowSOM and were systematically assessed for association with patient overall or progression-free survival. 43 glioblastoma cell subsets were identified and were color-coded based on hazard ratio of death and p-values (HR>1, red; HR<1, blue) Cell density, FlowSOM cluster, and cluster significance are depicted on t-SNE plots.
R Package Documentation
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We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
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