Biomarker Benchmark - GSE5460

Version 5 2016-03-17, 22:20

Version 4 2016-03-17, 21:28

Version 3 2016-02-23, 23:39

Version 2 2016-02-04, 22:37

Version 1 2016-02-02, 21:57

dataset

posted on 2016-03-17, 22:20 authored by Anna GuyerAnna Guyer, Stephen PiccoloStephen Piccolo

[NOTICE: This data set has been deprecated. Please see our new version of the data (and additional data sets) here: https://osf.io/mhk93 ]

"Predictors built from gene expression data accurately predict ER, PR, and HER2 status, and divide tumor grade into high-grade and low-grade clusters; intermediate-grade tumors are not a unique group. In contrast, gene expression data cannot be used to predict tumor size or lymphatic-vascular invasion.

Keywords: disease state analysis"

http://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE5460

We have included gene-expression data, the outcome (class) being predicted, and any clinical covariates. When gene-expression data were processed in multiple batches, we have provided batch information. Each data set is organized into a file set, where each contains all pertinent files for an individual dataset. The gene expression files have been normalized using both the SCAN and UPC methods using the SCAN.UPC package in Bioconductor (https://www.bioconductor.org/packages/release/bioc/html/SCAN.UPC.html). We summarized the data at the gene level using the BrainArray resource (http://brainarray.mbni.med.umich.edu/Brainarray/Database/CustomCDF/20.0.0/ensg.asp). We used Ensembl identifiers. The class, clinical, and batch data were hand curated to ensure consistency ("tidy data" formatting). In addition, the data files have been formatted to be imported easily into the ML-Flex machine learning package (http://mlflex.sourceforge.net/).