| Literature DB >> 26590402 |
Valerie Eichinger1, Thomas Nussbaumer1, Alexander Platzer1, Marc-André Jehl1, Roland Arnold2, Thomas Rattei3.
Abstract
Protein secretion systems play a key role in the interaction of bacteria and hosts. EffectiveDB (http://effectivedb.org) contains pre-calculated predictions of bacterial secreted proteins and of intact secretion systems. Here we describe a major update of the database, which was previously featured in the NAR Database Issue. EffectiveDB bundles various tools to recognize Type III secretion signals, conserved binding sites of Type III chaperones, Type IV secretion peptides, eukaryotic-like domains and subcellular targeting signals in the host. Beyond the analysis of arbitrary protein sequence collections, the new release of EffectiveDB also provides a 'genome-mode', in which protein sequences from nearly complete genomes or metagenomic bins can be screened for the presence of three important secretion systems (Type III, IV, VI). EffectiveDB contains pre-calculated predictions for currently 1677 bacterial genomes from the EggNOG 4.0 database and for additional bacterial genomes from NCBI RefSeq. The new, user-friendly and informative web portal offers a submission tool for running the EffectiveDB prediction tools on user-provided data.Entities:
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Year: 2015 PMID: 26590402 PMCID: PMC4702896 DOI: 10.1093/nar/gkv1269
Source DB: PubMed Journal: Nucleic Acids Res ISSN: 0305-1048 Impact factor: 16.971
Figure 1.Integration of methods for the prediction of bacterial secreted proteins and intact secretion systems in EffectiveDB. The workflow depicts the protein and genome modes of EffectiveDB. In the protein mode any set of proteins can be analyzed. The genome mode extends the protein mode by enabling EffectiveS346. For proteins from (almost) complete genomes the orthologous groups are calculated or provided by the user. These are the input data for the prediction of intact Type III, IV and VI secretion system.
Figure 2.Schematic output of EffectiveDB. The EffectiveDB output consists of predictions for individual proteins and for the entirety of proteins in a complete genome. Protein-based predictions (Type III secretion peptides, Type III chaperone binding sites, Type IV secretion peptides, eukaryotic-like domains and subcellular targeting) are grouped. Genome-based results are provided as summary and as lists of most relevant orthologous groups for each secretion system.