RT Journal Article SR Electronic T1 MetaSRA: normalized sample-specific metadata for the Sequence Read Archive JF bioRxiv FD Cold Spring Harbor Laboratory SP 090506 DO 10.1101/090506 A1 Bernstein, Matthew N. A1 Doan, AnHai A1 Dewey, Colin N. YR 2016 UL http://biorxiv.org/content/early/2016/12/19/090506.abstract AB Motivation The NCBI’s Sequence Read Archive (SRA) promises great biological insight if one could analyze the data in the aggregate; however, the data remain largely underutilized, in part, due to the poor structure of the metadata associated with each sample. The rules governing submissions to the SRA do not dictate a standardized set of terms that should be used to describe the biological samples from which the sequencing data are derived. As a result, the metadata include many synonyms, spelling variants, and references to outside sources of information. Furthermore, manual annotation of the data remains intractable due to the large number of samples in the archive. For these reasons, it has been difficult to perform large-scale analyses that study the relationships between biomolecular processes and phenotype across diverse diseases, tissues, and cell types present in the SRA.Results We present MetaSRA, a database of normalized SRA sample-specific metadata following a schema inspired by the metadata organization of the ENCODE project. This schema involves mapping samples to terms in biomedical ontologies, labeling each sample with a sample-type category, and extracting real-valued properties. We automated these tasks via a novel computational pipeline.Availability The MetaSRA database is available at http://deweylab.biostat.wisc.edu/metasra. Software implementing our computational pipeline is available at https://github.com/deweylab/metasra-pipeline.Contact cdewey{at}biostat.wisc.edu