Database Commons
Database Commons

a catalog of worldwide biological databases

Database Profile

ALE-HSA21

General information

URL: http://bioinfo.na.iac.cnr.it/ALE-HSA21/
Full name: AnaLysis of Expression of HSA21
Description: ALE-HSA21, AnaLysis of Expression of HSA21, is an integrated and a user-friendly relational database, which provides detailed information about various aspects of genes mapping on chromosome 21, such as gene structure, expression, nucleotide variations and association to diseases.
Year founded: 2014
Last update: 1/15/2014
Version: v1.0
Accessibility:
Accessible
Country/Region: Italy

Classification & Tag

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

Contact information

University/Institution: Institute of Genetics and Biophysics
Address: CNR, Naples, Italy
City: Naples
Province/State:
Country/Region: Italy
Contact name (PI/Team): Valerio Costa
Contact email (PI/Helpdesk): valerio.costa@igb.cnr.it

Publications

24573881
AnaLysis of Expression on human chromosome 21, ALE-HSA21: a pilot integrated web resource. [PMID: 24573881]
Scarpato M, Esposito R, Evangelista D, Aprile M, Ambrosio MR, Angelini C, Ciccodicola A, Costa V.

Transcriptome studies have shown the pervasive nature of transcription, demonstrating almost all the genes undergo alternative splicing. Accurately annotating all transcripts of a gene is crucial. It is needed to understand the impact of mutations on phenotypes, to shed light on genetic and epigenetic regulation of mRNAs and more generally to widen our knowledge about cell functionality and tissue diversity. RNA-sequencing (RNA-Seq), and the other applications of the next-generation sequencing, provides precious data to improve annotations' accuracy, simultaneously creating issues related to the variety, complexity and the size of produced data. In this 'scenario', the lack of user-friendly resources, easily accessible to researchers with low skills in bioinformatics, makes difficult to retrieve complete information about one or few genes without browsing a jungle of databases. Concordantly, the increasing amount of data from 'omics' technologies imposes to develop integrated databases merging different data formats coming from distinct but complementary sources. In light of these considerations, and given the wide interest in studying Down syndrome-a genetic condition due to the trisomy of human chromosome 21 (HSA21)-we developed an integrated relational database and a web interface, named ALE-HSA21 (AnaLysis of Expression on HSA21), accessible at http://bioinfo.na.iac.cnr.it/ALE-HSA21. This comprehensive and user-friendly web resource integrates-for all coding and noncoding transcripts of chromosome 21-existing gene annotations and transcripts identified de novo through RNA-Seq analysis with predictive computational analysis of regulatory sequences. Given the role of noncoding RNAs and untranslated regions of coding genes in key regulatory mechanisms, ALE-HSA21 is also an interesting web-based platform to investigate such processes. The 'transcript-centric' and easily-accessible nature of ALE-HSA21 makes this resource a valuable tool to rapidly retrieve data at the isoform level, rather than at gene level, useful to investigate any disease, molecular pathway or cell process involving chromosome 21 genes. Database URL: http://bioinfo.na.iac.cnr.it/ALE-HSA21/.

Database (Oxford). 2014:2014() | 11 Citations (from Europe PMC, 2025-12-20)

Ranking

All databases:
5136/6895 (25.526%)
Gene genome and annotation:
1541/2021 (23.8%)
Genotype phenotype and variation:
733/1005 (27.164%)
Structure:
707/967 (26.991%)
Health and medicine:
1277/1738 (26.582%)
5136
Total Rank
11
Citations
1
z-index

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Record metadata

Created on: 2015-06-20
Curated by:
Dong Zou [2018-03-08]
Mengwei Li [2016-03-31]
Mengwei Li [2016-03-28]
Mengwei Li [2015-11-23]
Mengwei Li [2015-06-26]