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Pathogenomics Goal: Identify previously unrecognized mechanisms of microbial pathogenicity using a unique combination of informatics, evolutionary biology, microbiology and genetics. Pathogenicity Processes of microbial pathogenicity at the molecular level are still minimally understood Pathogen proteins identified that manipulate host cells by interacting with, or mimicking, host proteins. Idea: Could we identify novel virulence factors by identifying pathogen genes more similar to host genes than you would expect based on phylogeny? Pathogens Anthrax Paratyphoid/enteric fever Cat scratch disease Peptic ulcers and gastritis Chlamydia Periodontal disease Cholera Plague Dental caries Pneumonia Diarrhea (E. coli etc.) Salmonellosis Diphtheria Scarlet fever Epidemic typhus Shigellosis (bacillary dysentery) Mediterranean fever Sleeping sickness Gastroenteritis Strep throat Giardia Syphilis Gonorrhea Toxic shock syndrome Legionnaires' disease Tuberculosis Leishmaniasis Tularemia Leprosy Typhoid fever Leptospirosis Urethritis Listeriosis Urinary Tract Infections Lyme disease Whooping cough Malaria Meningitis Necrotizing fasciitis Yeast infection Some hospital-acquired infections, animal/plant infections Approach Screen for candidate genes. Search pathogen genes against sequence databases. Identify those with notable similarity to eukaryotic genes. Rank candidates. - how much like host protein? - info available about protein? Evolutionary significance. - Horizontal transfer? Date of transfer? Coevolution? Similar by chance? Prioritize for further biological study. - Previously studied biologically? - Can UBC microbiologists study it? - C. elegans homolog? Modify screening method /algorithm Approach Prioritized candidates If C. elegans homolog - Target gene for knockout. - Analysis of knockout (expression chip, pathogen infection) - GFP fusion analysis C. elegans gene info continually exchanged with microbiologists If pathogen studied by UBC microbiologists - Obtain knockout - Analysis of knockout (expression chip, pathogenicity in C. elegans or other model - Subcellular localization If pathogen is not a focus of UBC group Contact other groups (possible collaboration) Pathogen gene info continually exchanged with eukaryotic geneticists Database: pathogen gene info (+ similar host/model host gene info) Interdisciplinary group Informatics/Bioinformatics Evolutionary Theory • Genome Sequence Centre, BC • Centre for Molecular Medicine and Therapeutics • Dept of Zoology • Dept of Botany • Canadian Institute for Advanced Research Pathogen Functions Host Functions • • • • • Dept. Medical Genetics • C. elegans Reverse Genetics Facility • Dept. Biological Sciences SFU Dept. Microbiology Biotechnology Laboratory Dept. Medicine BC Centre for Disease Control Power of the Approach • Interdisciplinary team unique ideas and collaborations • Expression-independent method • Automated approach continually updated • Better understanding: pathogen gene and similar host gene • Insight into horizontal gene transfer events and the evolution of pathogen-host interactions. • Public database – other researchers may capitalize on the findings – promote further collaboration Eukaryotic-like pathogen genes Aquifex aeolicus 96 Haemophilus influenza 100 Escherichia coli Anabaena - YopH, a proteintyrosine phosphatase, of Yersinia pestis 100 Synechocystis 100 63 Chlamydia trachomatis 64 Petunia x hybrida 83 0.1 Nicotiana tabacum Brassica napus 99 Arabidopsis thaliana 52 Oryza sativa - Enoyl-acyl carrier protein reductase (involved in lipid metabolism) of Chlamydia trachomatis Database front end for Pathogens Candidate proteins are ranked Customized blast result shows pair-wise distance and species information Customize the tree-building parameters View the constructed tree. Organism information is shown Also see prokaryotic-like proteins within Eukaryotic genomes Important if transfer is between a prokaryote and an eukaryotic parasite Bacterium Eukaryote Horizontal Transfer Trichomonas vaginalis Sialidase is 92-95% similar to Sialidase of Pasteurellaceae bacteria. Sialidase is a virulence factor used by some bacteria to parasitize the mucous membranes of animals. Peter Wall Major Thematic Grant • Fundamental research • Interdisciplinary • Major potential impact • Lack of fit with alternative funding sources Acknowledgements • Pathogenomics group – Ann M. Rose, Steven J. Jones, Yossef Av-Gay, David L. Baillie, Fiona S. L. Brinkman, Robert Brunham, Stefanie Butland, Rachel C. Fernandez, B. Brett Finlay, Robert E.W. Hancock, Christy Haywood-Farmer, Hans Greberg, Patrick Keeling, Audrey de Koning, Don G. Moerman, Sarah P. Otto, B. Francis Ouellette, Iain E. P. Taylor, Ivan Wan. • Peter Wall Foundation