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Predicting Protein Function Annotation using Protein-Protein Interaction Networks

Predicting Protein Function Annotation using Protein-Protein Interaction Networks. By Tamar Eldad Advisor: Dr. Yanay Ofran 89-385 Computational Biology - Projects Workshop Bar-Ilan University , the Mina and Everard Goodman Faculty of Life Sciences. Protein Function Prediction.

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Predicting Protein Function Annotation using Protein-Protein Interaction Networks

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  1. Predicting Protein Function Annotation using Protein-Protein Interaction Networks By Tamar Eldad Advisor: Dr. Yanay Ofran 89-385 Computational Biology - Projects Workshop Bar-Ilan University, the Mina and Everard Goodman Faculty of Life Sciences

  2. Protein Function Prediction • Exponential increase in the number of proteins being identified by sequence genomics projects • Impossible to perform functional assay for every uncharacterized gene • Turn to sophisticated computational methods for assistance in annotating the huge volume of sequence and structure data being produced • homology-based annotation transfer • sequence patterns • structure similarity • structure patterns • genomic context • microarray data

  3. What is Function? • Biological function has more than one aspect • Sub-cellular to whole-organism context • Physiological aspect • Phenotype The need of a well-defined vocabulary

  4. Protein Sequence: Protein Structure:

  5. The Gene Ontology The Gene Ontology project is a major bioinformatics initiative with the aim of standardizing the representation of gene and gene product attributes across species and databases. The project provides a controlled vocabulary of terms for describing gene product characteristics and gene product annotation data.

  6. The Gene Ontology Cellular component Molecular function Biological process DAG (1….N parent nodes) General  Specific Term is assigned to Gene Product

  7. The Gene Ontology

  8. A New Approach • Classical Biology – collect a set of features for each protein • Systems Biology – study protein function in the context of a network Assemblies represent more than the sum of their parts

  9. Protein Interactions • Data on thousands of interactions in humans and most model species have become available • mass spectrometry • genome-wide chromatin immunoprecipitation • yeast two-hybrid assays • combinatorial reverse genetic screens • rapid literature mining techniques

  10. PPI Networks Data are represented as networks, with nodes representing proteins and edges representing the detected PPIs.

  11. Existing Methods • Alignment – aligning sequence-matching proteins between species and checking if they also share network alignment can teach us about conserved pathways between species • Integration - data from different types of networks (i.e. protein, genetic, and transcriptional interaction networks) are integrated in order to get a better picture of the whole biological system • Querying - find sub-networks similar to functional units (by comparing interactions and the proteins themselves) - likely to be functioning units too

  12. New Method conserved network motifs between two species convey evidence for function similarity of the individual proteins that make up these motifs 1e-09 5e-15 8e-13 2e-10 HUMAN YEAST

  13. New Method What do we need? 1. list of proteins in human cell 2. list of proteins in yeast cell 3. interactions in each cell 4. sequence similarity grades 5. known GO annotations 6. function distance calculation

  14. Protein Lists - UniProt DB

  15. Interaction Databases • HPRD - The Human Protein Reference Database. • Dip - Database of Interacting Proteins. • Mips -Munich information center of proteins sequences • IntAct – interaction molecular database. • Reliable interaction performs one of these conditions: • 1. was at least observed in 2 different experiments. • OR • 2. was reported in 3 different articles.

  16. Sequence Similarity Grades BLAST - bl2seq HUMAN YEAST

  17. GO annotations –UniProt DB

  18. Evidence Codes

  19. Function Distance Calculation

  20. Implementation 1. Prepare similarity matrix for cutoff e-value 2. Find all components of size N – 1 (DFS search) 3. Compare sub-graphs found using similarity matrix 4. Add N-th non-similar component to each pair of matching graphs 5. Get GO function annotation of N-th components 6. Calculate average distance of N-th component’s function

  21. Quality Assurance • Compare to random-pair annotation • No-sequence similarity • Compare to sequence-similar annotation • BLAST • Only proteins under cut-off value • Human genes only

  22. Detailed Results

  23. Results E-value 5e-05

  24. Play with Parameters • Change graph size • Lower e-value • Start with larger amount of connected components • Use only graphs with higher connectivity • Non-similar proteins can be any protein in the graph • Different network topology • Limit number of paired proteins

  25. Results

  26. Conclusions Most results are random Significant improvement only for Biological Process prediction Still far behind Homology Based Transfer

  27. Summary • Functional annotation is one of the greatest challenges in the post-genomic era • PPI data for functional annotation as a new approach for promoting this field • Method tried out is unsuccessful • Other Ideas: • Find a more specific search pattern • Start from best results – what specializes them?

  28. References Friedberg,I. (2006) Automated function prediction: the genomic challenge. Brief. Bioinform. Accepted for publication Sharan R, Ulitsky I, Shamir R: Network-based prediction of protein function. Mol Syst Biol 2007, 3:88. Sharan R, Ideker T: Modeling cellular machinery through biological network comparison. Nature Biotechnology 24, 4: 427 - 433. http://www.geneontology.org/ http://www.chem.qmul.ac.uk/iubmb/enzyme/

  29. Thanks Advisor – Dr. Yanay Ofran Guys at the lab – Rotem, Vered, Sivan Roi Adadi & Omer Erel

  30. Alignment

  31. Querying

  32. Integration

  33. Similarity Matrix E-value = 0.0005 HUMAN YEAST TRUE TRUE FALSE FALSE FALSE FALSE

  34. Neighboring matrix HUMAN CELL INTERACTIONS

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