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Database Commons

a catalog of worldwide biological databases

Database Profile

SignaLink

General information

URL: http://SignaLink.org
Full name: signaling pathways reveal tissue-specific cross-talks
Description: An integrated resource to analyze signaling pathway cross-talks, transcription factors, miRNAs and regulatory enzymes
Year founded: 2010
Last update: 2022-03-01
Version: 3.1
Accessibility:
Accessible
Country/Region: Hungary

Classification & Tag

Data type:
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Contact information

University/Institution: Eötvös University
Address:
City:
Province/State:
Country/Region: Hungary
Contact name (PI/Team): Tamás Korcsmáros
Contact email (PI/Helpdesk): korcsmaros@netbiol.elte.hu

Publications

34634810
SignaLink3: a multi-layered resource to uncover tissue-specific signaling networks. [PMID: 34634810]
Csabai L, Fazekas D, Kadlecsik T, Szalay-Bekő M, Bohár B, Madgwick M, Módos D, Ölbei M, Gul L, Sudhakar P, Kubisch J, Oyeyemi OJ, Liska O, Ari E, Hotzi B, Billes VA, Molnár E, Földvári-Nagy L, Csályi K, Demeter A, Pápai N, Koltai M, Varga M, Lenti K, Farkas IJ, Türei D, Csermely P, Vellai T, Korcsmáros T.

Signaling networks represent the molecular mechanisms controlling a cell's response to various internal or external stimuli. Most currently available signaling databases contain only a part of the complex network of intertwining pathways, leaving out key interactions or processes. Hence, we have developed SignaLink3 (http://signalink.org/), a value-added knowledge-base that provides manually curated data on signaling pathways and integrated data from several types of databases (interaction, regulation, localisation, disease, etc.) for humans, and three major animal model organisms. SignaLink3 contains over 400 000 newly added human protein-protein interactions resulting in a total of 700 000 interactions for Homo sapiens, making it one of the largest integrated signaling network resources. Next to H. sapiens, SignaLink3 is the only current signaling network resource to provide regulatory information for the model species Caenorhabditis elegans and Danio rerio, and the largest resource for Drosophila melanogaster. Compared to previous versions, we have integrated gene expression data as well as subcellular localization of the interactors, therefore uniquely allowing tissue-, or compartment-specific pathway interaction analysis to create more accurate models. Data is freely available for download in widely used formats, including CSV, PSI-MI TAB or SQL.

Nucleic Acids Res. 2021:() | 29 Citations (from Europe PMC, 2025-12-20)
20542890
Uniformly curated signaling pathways reveal tissue-specific cross-talks and support drug target discovery. [PMID: 20542890]
Korcsmáros T, Farkas IJ, Szalay MS, Rovó P, Fazekas D, Spiró Z, Böde C, Lenti K, Vellai T, Csermely P.

MOTIVATION: Signaling pathways control a large variety of cellular processes. However, currently, even within the same database signaling pathways are often curated at different levels of detail. This makes comparative and cross-talk analyses difficult.
RESULTS: We present SignaLink, a database containing eight major signaling pathways from Caenorhabditis elegans, Drosophila melanogaster and humans. Based on 170 review and approximately 800 research articles, we have compiled pathways with semi-automatic searches and uniform, well-documented curation rules. We found that in humans any two of the eight pathways can cross-talk. We quantified the possible tissue- and cancer-specific activity of cross-talks and found pathway-specific expression profiles. In addition, we identified 327 proteins relevant for drug target discovery.
CONCLUSIONS: We provide a novel resource for comparative and cross-talk analyses of signaling pathways. The identified multi-pathway and tissue-specific cross-talks contribute to the understanding of the signaling complexity in health and disease, and underscore its importance in network-based drug target selection.
AVAILABILITY: http://SignaLink.org.

Bioinformatics. 2010:26(16) | 59 Citations (from Europe PMC, 2025-12-20)

Ranking

All databases:
2225/6895 (67.745%)
Pathway:
140/451 (69.18%)
2225
Total Rank
83
Citations
5.533
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Record metadata

Created on: 2018-01-29
Curated by:
Yuxin Qin [2022-05-09]
Yang Zhang [2018-02-23]