APPRIS: annotation of principal and alternative splice isoforms.

paper Cited Public

Authors: Rodriguez, Jose Manuel; Maietta, Paolo; Ezkurdia, Iakes; Pietrelli, Alessandro; Wesselink, Jan-Jaap; Lopez, Gonzalo; Valencia, Alfonso; Tress, Michael L
Year: 2013
Journal: Nucleic acids research
PMID: 23161672
DOI: 10.1093/nar/gks1058
PMCID: PMC3531113

Figure 1.

The APPRIS system. The inputs to the web services are the peptide sequences of the isoforms, the sequences of the transcripts and cross-species alignments of either transcripts or peptides. The output of all eight individual web services is used by APPRIS to annotate alternative variants with structural, functional and conservation information and to select a principal isoform for each gene.

Figure 2.

APPRIS annotations for gene DNAJC5G. (A) Snapshot of the APPRIS page for gene DNAJC5G, showing the five protein-coding transcripts annotated by Ensembl and the selection of the principal isoform by APPRIS (shown by the green tick). (B) A selection of the annotation results from the individual modules in APPRIS (Matador3D maps 3D structure to the isoforms, SPADE maps Pfam functional domains and INERTIA detects unusually evolving exons). The principal isoform is highlighted. APPRIS chooses isoform DNAJC5G-004 as the main variant based on the output of SPADE and Matador3D and designates the two ‘KNOWN’ isoforms (which are also CCDS variants) as alternative variants. (C) The 3D structure of mouse DNAJ subfamily C2 member 5 (PDB: 2CTW), to which DNAJC5G-004 has 56% identity with no gaps. The coloring on the 3D structure comes from the predominant coloring in the Pfam multiple alignment in (D). The large red arrow shows that the 16 extra residues present in the larger isoforms would have to be inserted into an important helix. (D) The multiple alignment for a section of the Pfam DnaJ family of sequences. The red arrow shows that the 16 extra residues in the CCDS variants would need to be inserted into a critical region of the functional domain of DNAJC5G.

Figure 3.

APPRIS result for gene TP63. (A) The four variants of gene TP63 that score highest in APPRIS, highlighting the 5′-splice junction differences between TA and P63delta, deltaN and TP63-013, and the GYNGYN splice event that differentiates TA and deltaN from P63delta and TP63-013. (B) Annotation results from some of the individual modules in APPRIS (Matador3D maps 3D structure to the isoforms, SPADE maps Pfam functional domains and CORSAIR detects orthologous isoforms in related species). The isoforms are color-coded as in (A) and we have added two other well-known TP63 variants to the table. APPRIS chooses isoform TP63-013 as the main variant based on the output of the three modules.

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40	FUNDING	Conflict of interest statement. None declared.

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Framework and resource for more than 11,000 gene-transcript-protein-reaction associations in human metabolism.	Ryu JY et al.	—	2017	→
Mapping, modeling, and characterization of protein-protein interactions on a proteomic scale.	Cafarelli TM et al.	—	2017	→
Pre-mRNA mis-splicing of sarcomeric genes in heart failure.	Zhu C et al.	—	2017	→
Transcription factor-DNA binding: beyond binding site motifs.	Inukai S et al.	—	2017	→
CRISPR knockout screening outperforms shRNA and CRISPRi in identifying essential genes.	Evers B et al.	—	2016	→
Extreme genomic erosion after recurrent demographic bottlenecks in the highly endangered Iberian lynx.	Abascal F et al.	—	2016	→
Plastid: nucleotide-resolution analysis of next-generation sequencing and genomics data.	Dunn JG et al.	—	2016	→
PPIXpress: construction of condition-specific protein interaction networks based on transcript expression.	Will T et al.	—	2016	→
The BLUEPRINT Data Analysis Portal.	Fernández JM et al.	—	2016	→
The Ensembl Variant Effect Predictor.	McLaren W et al.	—	2016	→
The state of play in higher eukaryote gene annotation.	Mudge JM et al.	—	2016	→
Towards improved genome-scale metabolic network reconstructions: unification, transcript specificity and beyond.	Pfau T et al.	—	2016	→
Trisomy 21 Alters DNA Methylation in Parent-of-Origin-Dependent and -Independent Manners.	Alves da Silva AF et al.	—	2016	→
Alternatively Spliced Homologous Exons Have Ancient Origins and Are Highly Expressed at the Protein Level.	Abascal F et al.	—	2015	→
APPRIS WebServer and WebServices.	Rodriguez JM et al.	—	2015	→
Cis-Expression Quantitative Trait Loci Mapping Reveals Replicable Associations with Heroin Addiction in OPRM1.	Hancock DB et al.	—	2015	→
Comparison of GENCODE and RefSeq gene annotation and the impact of reference geneset on variant effect prediction.	Frankish A et al.	—	2015	→
Creating reference gene annotation for the mouse C57BL6/J genome assembly.	Mudge JM et al.	—	2015	→
Functional Networks of Highest-Connected Splice Isoforms: From The Chromosome 17 Human Proteome Project.	Li HD et al.	—	2015	→
Identifying and characterising key alternative splicing events in Drosophila development.	Lees JG et al.	—	2015	→
Integrative analysis of RNA, translation, and protein levels reveals distinct regulatory variation across humans.	Cenik C et al.	—	2015	→
miRGate: a curated database of human, mouse and rat miRNA-mRNA targets.	Andrés-León E et al.	—	2015	→
MIsoMine: a genome-scale high-resolution data portal of expression, function and networks at the splice isoform level in the mouse.	Li HD et al.	—	2015	→
Most highly expressed protein-coding genes have a single dominant isoform.	Ezkurdia I et al.	—	2015	→
Potential Gene Interactions in the Cell Cycles of Gametes, Zygotes, Embryonic Stem Cells and the Development of Cancer.	Prindull G	—	2015	→
Reconstruction of genome-scale human metabolic models using omics data.	Ryu JY et al.	—	2015	→
Semi-supervised Learning Predicts Approximately One Third of the Alternative Splicing Isoforms as Functional Proteins.	Hao Y et al.	—	2015	→
Structure-PPi: a module for the annotation of cancer-related single-nucleotide variants at protein-protein interfaces.	Vázquez M et al.	—	2015	→
The distribution pattern of genetic variation in the transcript isoforms of the alternatively spliced protein-coding genes in the human genome.	Liu T et al.	—	2015	→
Tissue-Specific Evolution of Protein Coding Genes in Human and Mouse.	Kryuchkova-Mostacci N et al.	—	2015	→
Analysis of stop-gain and frameshift variants in human innate immunity genes.	Rausell A et al.	—	2014	→
Diversity and evolution of membrane intrinsic proteins.	Abascal F et al.	—	2014	→
Multiple evidence strands suggest that there may be as few as 19,000 human protein-coding genes.	Ezkurdia I et al.	—	2014	→
Revisiting the identification of canonical splice isoforms through integration of functional genomics and proteomics evidence.	Li HD et al.	—	2014	→
SIBIS: a Bayesian model for inconsistent protein sequence estimation.	Khenoussi W et al.	—	2014	→
Alternative splicing for diseases, cancers, drugs, and databases.	Tang JY et al.	—	2013	→
Systematically differentiating functions for alternatively spliced isoforms through integrating RNA-seq data.	Eksi R et al.	—	2013	→
The alternative heart: impact of alternative splicing in heart disease.	Lara-Pezzi E et al.	—	2013	→
The impact of splicing on protein domain architecture.	Light S et al.	—	2013	→
Transcriptome analysis of human tissues and cell lines reveals one dominant transcript per gene.	Gonzàlez-Porta M et al.	—	2013	→