The Bader lab aims to develop a computational cell map that organizes all biological processes and their component interactions and molecules. This map can then be read to understand how biological processes work, what is the function of a gene, and what effects disease-associated or engineered mutations have. Cell maps from different organisms or cell types can be compared to identify important components. Three research tracks and one software infrastructure track are actively developing to reach this goal.

Research Tracks

Genome to Network

We are developing computational methods to accurately predict the binding specificity of peptide recognition domains given the domain sequence and to predict biologically relevant protein-protein interactions given binding specificity. We are focusing on PDZ domains, recognizing hydrophobic C-termini, and WW and SH3 domains, recognizing proline rich motifs. Our questions are:

Team: David Gfeller, Shirley Hui, Chris Tan
Collaborators: Sachdev Sidhu, Charlie Boone, Tony Pawson, Marius Sudol, Chris Sander
Funding: CIHR

Active Cell Map

The 'active cell map' is the set of all interactions, complexes and pathways involving molecules in the cell and their activity under normal and diseased regulatory circumstances. We are developing novel computational methods to combine molecular network and profiles to uncover active cell map regions. Our questions are:

Team: Daniele Merico, Vuk Pavlovic, Ruth Isserlin
Collaborators: Andrew Emili, Anthony Gramolini
Funding: CFI/MRI

Multiple Perturbation Mapping

Buffering between biological processes, like the cell cycle and DNA damage repair systems, underlies cellular robustness to perturbations. Defects in one system affect dependent, but not buffered systems. Identifying these relationships is useful to delineate system boundaries in the cell. We aim to use quantitative genetic interactions to define pathways and complexes and infer their detailed buffering relationships. Our questions are:

Team: Anastasia Baryshnikova, Iain Wallace, Laetitia Morrison, Magali Michaut
Collaborators: Charlie Boone, Brenda Andrews, Guri Giaever, Corey Nislow
Funding: NSERC, Genome Canada Integrative Biology of Yeast

References:

  1. Global Mapping of the Yeast Genetic Interaction Network Tong AH, Lesage G, Bader GD, Ding H, Xu H, Xin X, Young J, Berriz GF, Brost RL, Chang M, Chen Y, Cheng X, Chua G, Friesen H, Goldberg DS, Haynes J, Humphries C, He G, Hussein S, Ke L, Krogan N, Li Z, Levinson JN, Lu H, Menard P, Munyana C, Parsons AB, Ryan O, Tonikian R, Roberts T, Sdicu AM, Shapiro J, Sheikh B, Suter B, Wong SL, Zhang LV, Zhu H, Burd CG, Munro S, Sander C, Rine J, Greenblatt J, Peter M, Bretscher A, Bell G, Roth FP, Brown GW, Andrews B, Bussey H, Boone C Science 2004 Feb 6;303(5659):808-813 - PubMed Abstract - PDF - Science Perspective PDF

  2. Systematic Genetic Analysis with Ordered Arrays of Yeast Deletion Mutants Tong AH, Evangelista M, Parsons AB, Xu H, Bader GD, Page N, Robinson M, Raghibizadeh S, Hogue CW, Bussey H, Andrews B, Tyers M, Boone C Science 2001 Dec 14;294(5550):2364-8 - PubMed Abstract - PDF

Software Infrastructure Track

More details on the Software page.

Pathway Commons

Pathway Commons is a collection of publicly available pathways from multiple organisms. It provides researchers with convenient access to a comprehensive collection of pathways from multiple sources represented in a common language (BioPAX). Pathways are stored in the cPath database software. URL: http://www.pathwaycommons.org Pathway Commons is developed in collaboration with Chris Sander's group at MSKCC.

Cytoscape

Cytoscape is an open source bioinformatics software platform for visualizing molecular interaction networks and integrating these interactions with gene expression profiles and other state data. URL: http://cytoscape.org/

Team: Rashad Badrawi, Ovi Comes, Khalid Zuberi, Jason Montojo, Christian Lopes, Sylva Donaldson
Collaborators: Chris Sander (MSKCC), Quaid Morris (UofT), Trey Ideker (UCSD), Benno Schwikowski (Pasteur), David States (UMich), Annette Adler (Agilent), Yeyejide Adelye (Unilever), Bruce Conklin (UCSF), Lee Hood and Ilya Schmulevich (ISB).  Many other Cytoscape, BioPAX and PSI-MI community members are important for this work.
Funding: NIH NHGRI, Genome Canada Technology Development

Full funding details at Funding

Research (last edited 2009-07-23 16:48:03 by MagaliMichaut)

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