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Genomics in Drug Discovery

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Title: Genomics in Drug Discovery


1
Genomics in Drug Discovery
  • _at_ Organon, Oss
  • 2005-08-22
  • Tim Hulsen

2
Introduction
  • Proteins are vital to life
  • involved in all kinds of life processes
  • Understanding protein functions
  • and relationships is very important for
  • drug design
  • Currently, the molecular function of about
  • 40 of the proteins is unknown

3
Introduction
Availability of fully sequenced genomes gives us
a wealth of information currently more than 15
eukaryotic genomes have nearly been completely
sequenced, over 148 microbial genomes and over
1000 viruses.
  • Determine protein function by using different in
    silico techniques
  • sequence comparison to known protein sequences
  • sequence clustering with proteins which have the
    same or similar function

4
Genomics _at_ OrganonThe Protein World project
  • All-against-all sequence comparison of complete
    proteomes from 145 species
  • Smith-Waterman algorithm Z-value (Monte-Carlo
    statistics)

5
Protein World and its ambitions
  • Build and maintain a sequence similarity
    repository of all complete proteomes and aligning
    it with omics research in the Netherlands
  • Classification of all proteins into groups of
    related proteins
  • A phylogenetic repository
  • Annotation of new sequences
  • Mining protein families
  • Identification of genes common / specific to
    (groups of) species

6
Applications of Protein World
  • Structural properties
  • Protein comparison coupled to structure related
    databases (PDB, SCOP, etc.)
  • Systems biology
  • Connecting PW to other databases (pathways,
    protein interactions, literature etc.)
  • Orthology
  • Annotation of new proteins
  • To predict discrepancies and similarities between
    species

7
Orthology
  • Describes the evolutionary relationship between
    homologous genes whose independent evolution
    reflects a speciation event (Fitch, 1970)

8
Protein World Drug Discovery
  • Orthologies can be used to transfer function of
    proteins in model organisms (mice, rats, dogs,
    etc.) to humans
  • Drugs tested on model organisms can have
    different effects in humans. Why?
  • Could be explained by looking at proteins in drug
    pathways and their orthologs
  • Example trypsin inhibition pathway

9
Trypsin inhibition pathway (1)
  • Organon thrombin inhibitors
  • Needed to stop thrombosis (blood clotting)
  • Thrombin inhibitor on the market (xi)melagatran,
    sold as Exanta (AstraZeneca)
  • Proven to be better than warfarin, but

10
Trypsin inhibition pathway (2)
  • Side effect of thrombin inhibitors inhibition of
    trypsin
  • Trypsin inhibition -gt rise in cholecystokinin
    (CCK) levels -gt stimulation of pancreas -gt
    pancreatic tumors
  • Difficult to test in model organisms
  • Rat very strong CCK response
  • Mouse weak CCK response
  • Human almost no CCK response

11
Trypsin inhibition pathway (3)
12
Trypsin inhibition pathway (4)
  • Ortholog identification methods
  • Using functional annotation (SPTrEMBL)
  • Best Bidirectional Hit (BBH)
  • ? one-to-one relationships
  • PhyloGenetic Trees (PGT)
  • ? many-to-many relationships

13
Best Bidirectional Hit (BBH)
  • Very easy and quick
  • Human protein (1) ? SW ? best hit in mouse/rat
    (2)
  • Mouse/rat protein (2) ? SW ? best hit in human
    (3)
  • If 3 equals 1, the human and mouse/rat protein
    are considered to be orthologs

14
PhyloGenetic Tree (PGT)
  • Human
  • All
  • eukaryotic
  • proteomes
  • Zgt20
    RHgt0.5QL
  • 25,000
    groups

PROTEOME
Hs-Mm pairs Hs-Rn pairs
TREE SCANNING
15
Trypsin inhibition pathway (5)
  • Mm Hs Rn
  • by annotation
  • BBH
  • PGT

16
Trypsin inhibition pathway (6)
  • PGT method in some cases too many orthologous
    relationships, especially for trypsin (73 in
    mouse and 62 in rat!)
  • BBH method seems to be more usable for this
    study, but still not gives an explanation for the
    differences in CCK levels
  • Our problem (different CCK responses in Human,
    Mouse and Rat) cannot be solved only by orthology
    identification
  • ? Combine ortholog analysis with other data
  • ? Focus on the molecules that are most likely to
    be responsible for these differences CCK and
    trypsin

17
Trypsin inhibition pathway (7)
  • Current activities
  • Take a better look at regulation promoter
    detection?
  • Use expression data?
  • Structural explanation? Modelling of interactions
    between the involved molecules

18
Possible student projects
  • Orthology case study explain differences between
    humans and model organisms
  • (like example of trypsin inhibition pathway)
  • Chicken project (in collaboration with Wageningen
    University) comparison of immune system in
    chickens to i.s. in humans and other vertebrates
  • Cluster algorithms

19
People
  • Peter Groenen
  • Wilco Fleuren
  • Tim Hulsen
  • Others _at_ MDI
  • Students?
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