Lec 5- Target discovery (2) Flashcards
1
Q
Genome and proteome approaches
A
2
Q
Proteomics
A
- Proteomics: The study of the complete protein complement of a cell (or sub-fracrtion thereof e.g. isolate organelle)
- Comparison of diseased vs healthy cells, infectious vs non-infectious etc, and the identification of the proteins responsible
- More informative than the geonme (Drosophila genome 15,000 genes, human genome 22,000 genes) but how many proteins
- Relies on genome information and integration of information from a wide variety of sources
3
Q
Differential proteomics
A
- Cellular level phenotypes- is it proliferating more than usual
- Induce bad sample
- Clinical- compare healthy and diseased tissue- cancer v non-cancer
- Seperate out proteins- what is different between them
- Quantify and analyse and identify differences
4
Q
2D-page
2D gel electrophoresis
A
- Separate proteins by isoelectric point- pH at which the charge of AA is neutral- (pl) in the first dimension (Isoelectric focusing on an immobilized pH gradient)
- Then separate by size in the second (12% SDS)
5
Q
A
- We can us MS to identify the proteins
- Down = glycosis= making energy
- Up= these proteins protect the cell from oxygen
- Oxidative damage to proteins is linked to neurodegeneration
6
Q
Proteomics
A
- Benzamide inhibits tumour growth
- H1299 cells treated with bengamideanalogue LAF389
- Proteins extracted and separated
- Identify the proteins that change- 14-3-3 isoforms
- Relate to biochemistry- inhibits methionine aminopeptidase
- Start codon contains methionine, every protein starts with methionine and is removed once started, aminopeptidase cleaves this- by inhibiting aminopeptidase we cause the production of lots of inactive proteins= cancer cell dies
- New targets for developing assays and drugs
7
Q
Chemical proteomics
A
- Many drugs have been discovered by screening but their target is often not known
- Chemical proteomics uses the drug as a bait to capture the proteins that bind to the drug
- The target and off-target proteins can be identified
- We attach the drug to a magnetic particle to access it easily
- We allow the drug to bind to any targets (enzymes, proteins) that it can
- On removal those proteins should still be bound
- We can then identify the protein
- It could be target that causes action- on target
- Target could cause side effect (we dont want it to bind to that protein)- off target
8
Q
Chemical proteomics: examples- trapoxin
A
Trapoxin
- A fungal product identified as an anti-cancer agent found to bind to histone deacetylase (HDAC)- packing and unpackaging DNA, control expression of DNA
- Shown to be a HDAC inhibitor- led to an understanding of epigenetics
- This led directly to the development of the clinically used HDAC inhibitors suberoylanilide hydroxamic acid (SAHA) and Romidepsin (FK228) for the treatment of lymphoma
9
Q
chemical proteomics- example thalidomide
A
- Very effective sedative and treatment for morning sickness
- Withdrawn 1961 due to teratogenicity
- In 2010 the molecular basis for this was uncovered to be cereblon which is involved in the expression of growth factors
- Development of new analogues that avoid this interaction
10
Q
Induced phenotypic approaches- Take a model organism
A
- Take a model organism
- Mutate it (chemically) and look for the disease like phenotypes
- Identify the gene that is changed by sequencing the genome
- Use RNAi to ‘silence’ genes and look for the disease like phenotypes
- NB- RNAi- small double-stranded RNA that are put into cells and produce siRNA (single-stranded) that interacts with the cellular mRNA and prevent the gene product being formed
11
Q
An example from genomics
A
- Genomics allows the study of the full gene complement of a system
- The Her2 gene (ErbB, epidermal growth factor receptor family) was identified as an oncogene in a model using chemically induced rat neuroblastoma in 1984
- Found to be overexpressed in <25% of breast carcinoma
- Kohler and Milstein had discovered the use use of Ab’s in therapy in 1975- approach used to develop Herceptin
- Trastuzumab (1988) developed as therapy, approved 2005
12
Q
Technology can deliver new knowledge and understanding
A
- The general belief is that around 3% of the human genomic DNA codes for protein products
- Evidence from total transcribed genome analysis suggested that there may be a large amount (possibly as much again) DNA being transcribed as was previously predicted
- Discovery of micro-RNA
- Is it meaningful?
13
Q
Chemical genetics
A
- Nothing new- aspirin from willow bark but not until 1970 that target identified- led to new analgesics
- Rapamycin- from Streptomyces hygroscopicus in 1970s as antifungal found to inhibit mTOR
- Current methods involve screening for a compound that gives a desired phenotype
- Monastrol identified as antimitotic (from >16,000 compounds)
- Using a screen to look at distribution of H-Ras and Raf1 >73,000 compounds screened and one compound identified- MCP1
14
Q
Systems biology and systems medicine
A
- While looking at individual targets allows us to develop specific pharmaceuticals, it is common for resistance to develop or of-target effects to become apparent after time
- System biology and systems medicine aim at look at a whole biological system, and to develop functional models that allow us to predict the effects of chanhing one component e.g. targeting one protein
- Also aim to develop systems wide screens for identifying biomarker patterns that can be used in diagnosis and monitoring of treatment
15
Q
Drug fail
A
- Very expensive to fail in phase I and II clinical trials- one of the reasons why drugs are so expensive
- We can use these approaches to target discovery we can screen for much more effective drugs, as well as potentially identify why it fails to make the whole process more efficient
