Database Commons
Database Commons

a catalog of worldwide biological databases

Database Profile

H-DBAS

General information

URL: http://h-invitational.jp/h-dbas/
Full name: Human-transcriptome Database for Alternative Splicing
Description: H-DBAS is a specialized database for human alternative splicing (AS) based on H-Invitational full-length cDNAs.
Year founded: 2007
Last update: 2010-09-09
Version: v6.0
Accessibility:
Accessible
Country/Region: Japan

Classification & Tag

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

Contact information

University/Institution: National Institute of Advanced Industrial Science and Technology
Address: AIST Bio-IT Research Bldg. Aomi 2-4-7, Koto-ku, Tokyo 135-0064, Japan
City: Tokyo
Province/State:
Country/Region: Japan
Contact name (PI/Team): Tadashi Imanishi
Contact email (PI/Helpdesk): t.imanishi@aist.go.jp

Publications

19969536
H-DBAS: human-transcriptome database for alternative splicing: update 2010. [PMID: 19969536]
Takeda J, Suzuki Y, Sakate R, Sato Y, Gojobori T, Imanishi T, Sugano S.

H-DBAS (http://h-invitational.jp/h-dbas/) is a specialized database for human alternative splicing (AS) based on H-Invitational full-length cDNAs. In this update, for better annotations of AS events, we correlated RNA-Seq tag information to the AS exons and splice junctions. We generated a total of 148,376,598 RNA-Seq tags from RNAs extracted from cytoplasmic, nuclear and polysome fractions. Analysis of the RNA-Seq tags allowed us to identify 90,900 exons that are very likely to be used for protein synthesis. On the other hand, 254 AS junctions of human RefSeq transcripts are unique to nuclear RNA and may not have any translational consequences. We also present a new comparative genomics viewer so that users can empirically understand the evolutionary turnover of AS. With the unique experimental data closely connected with intensively curated cDNA information, H-DBAS provides a unique platform for the analysis of complex AS.

Nucleic Acids Res. 2010:38(Database issue) | 28 Citations (from Europe PMC, 2025-03-29)
17130147
H-DBAS: alternative splicing database of completely sequenced and manually annotated full-length cDNAs based on H-Invitational. [PMID: 17130147]
Takeda J, Suzuki Y, Nakao M, Kuroda T, Sugano S, Gojobori T, Imanishi T.

The Human-transcriptome DataBase for Alternative Splicing (H-DBAS) is a specialized database of alternatively spliced human transcripts. In this database, each of the alternative splicing (AS) variants corresponds to a completely sequenced and carefully annotated human full-length cDNA, one of those collected for the H-Invitational human-transcriptome annotation meeting. H-DBAS contains 38,664 representative alternative splicing variants (RASVs) in 11,744 loci, in total. The data is retrievable by various features of AS, which were annotated according to manual annotations, such as by patterns of ASs, consequently invoked alternations in the encoded amino acids and affected protein motifs, GO terms, predicted subcellular localization signals and transmembrane domains. The database also records recently identified very complex patterns of AS, in which two distinct genes seemed to be bridged, nested or degenerated (multiple CDS): in all three cases, completely unrelated proteins are encoded by a single locus. By using AS Viewer, each AS event can be analyzed in the context of full-length cDNAs, enabling the user's empirical understanding of the relation between AS event and the consequent alternations in the encoded amino acid sequences together with various kinds of affected protein motifs. H-DBAS is accessible at http://jbirc.jbic.or.jp/h-dbas/.

Nucleic Acids Res. 2007:35(Database issue) | 30 Citations (from Europe PMC, 2025-03-29)

Ranking

All databases:
2479/6278 (60.529%)
Expression:
506/1214 (58.402%)
2479
Total Rank
56
Citations
3.294
z-index

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Record metadata

Created on: 2015-07-14
Curated by:
Lin Liu [2022-08-20]
Fatima Batool [2018-12-27]
Lina Ma [2018-06-12]
Chunlei Yu [2016-04-27]
Chunlei Yu [2016-03-31]
Chunlei Yu [2015-11-19]