Database Commons
Database Commons

a catalog of worldwide biological databases

Database Profile

General information

URL: https://structurome.bb.iastate.edu
Full name: RNA Structurome Database
Description: RNA Structurome Database is a comprehensive repository of RNA secondary structural information that spans the entire human genome. These data will facilitate a wide array of investigations: e.g. discovery of structured regulatory elements in differential gene expression data or noncoding RNA discovery, as well as allow genome-scale analyses of RNA folding.
Year founded: 2017
Last update:
Version: 26
Accessibility:
Manual:
Accessible
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Country/Region: United States

Classification & Tag

Data type:
DNA
Data object:
Database category:
Major species:
Keywords:

Contact information

University/Institution: Iowa State University
Address: Roy J. Carver Department of Biochemistry, Biophysics, and Molecular Biology, Iowa State University, 2437 Pammel Drive, Ames, IA 50011 USA
City: Ames
Province/State:
Country/Region: United States
Contact name (PI/Team): Walter N. Moss
Contact email (PI/Helpdesk): wmoss@iastate.edu

Publications

29222504
RNAStructuromeDB: A genome-wide database for RNA structural inference. [PMID: 29222504]
Andrews RJ, Baber L, Moss WN.

RNA plays important roles in almost every aspect of biology, and every aspect of RNA biology is influenced by its folding. This is a particularly important consideration in the era of high-throughput sequencing, when the discovery of novel transcripts far outpaces our knowledge of their functions. To gain a comprehensive picture of biology requires a structural framework for making functional inferences on RNA. To this end we have developed the RNA Structurome Database ( https://structurome.bb.iastate.edu ), a comprehensive repository of RNA secondary structural information that spans the entire human genome. Here, we compile folding information for every base pair of the genome that may be transcribed: coding, noncoding, and intergenic regions, as well as repetitive elements, telomeres, etc. This was done by fragmenting the GRCh38 reference genome into 154,414,320 overlapping sequence fragments and, for each fragment, calculating a set of metrics based on the sequence's folding properties. These data will facilitate a wide array of investigations: e.g. discovery of structured regulatory elements in differential gene expression data or noncoding RNA discovery, as well as allow genome-scale analyses of RNA folding.

Sci Rep. 2017:7(1) | 27 Citations (from Europe PMC, 2024-04-20)

Ranking

All databases:
619/6000 (89.7%)
Gene genome and annotation:
216/1675 (87.164%)
619
Total Rank
27
Citations
3.857
z-index

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Record metadata

Created on: 2018-01-29
Curated by:
Saba Arshad [2018-04-13]
Yang Zhang [2018-01-28]