Post on 02-Jan-2016
Computational biology of cancer cell pathways
Modelling of cancer cell function and response to therapy
Signalling pathways
Signal from outside cell
Signal from inside cell
Source: Biocarta database
Epidermal growth factor (EGF) signalling
Signal from outside cell
Gene expression
Signal from outside or inside cell
Signal transmitted to genome
Changes in gene expression = cell
response to signal
Information about cell’s environment
and internal state is coupled to gene
expression
Signalling pathways
Receptors
E.g., kinases
Transcription factors
Mutations in cancer
• Point mutations - changes in protein sequence or control sequences
• Genome instability: Loss or gain of single genes or chromosome portions (many genes)
Abnormal amounts of proteins
Abnormal function, e.g always ‘switched on’ or inactivated
Signalling pathways in cancer cells
Mutations in cancer
• Point mutations - changes in protein sequence or control sequences
• Genome instability: Loss or gain of single genes or chromosome portions (many genes)
Abnormal amounts of proteins
Abnormal function, e.g always ‘switched on’ or inactivated
Changes in information processing underpin hallmarks of
cancer
Signalling pathways in cancer cells
Signalling pathwaysin cancer cells
Epidermal growth factor receptor (EGFR)
• Overexpression of EGFR is common in many solid tumours
• Correlates with increased metastasis, decreased survival and a poor prognosis
• Protects malignant tumour cells from the cytotoxic effects of chemotherapy and radiotherapy, making these treatments less effective
EGFR is the target for several new anticancer therapies
EGFR-targeted therapy
cell surface portion
binds epidermal growth factorintracellular tyrosine kinase transmit signal by phosphorylation
CE
LL M
EM
BR
AN
E
EGFR-targeted therapy
Small molecule inhibitors
Therapeutic antibody: Cetuximab (colorectal cancer)
Inhibition of EGFR
• Both types of inhibitors block signalling from the EGF receptor
• Inhibition limits tumour growth, dissemination, angiogenesis
• Reduces resistance to chemotherapy and radiotherapy
• Aids the induction of cell death (apoptosis)
Not a linear pathway, but a complex network
Genome
Growth factor (EGF)
Receptor tyrosine kinase
PLC Ras PI3K
PKC MAPK PKB/Akt
TFs Functional targets
CELL GROWTH AND PROLIFERATION
ERK
Cross-activation by other pathways
Not a linear pathway, but a complex network
Signal processing by the entire network and mutations or expression changes in signal proteins can limit response to therapy or cause side effects.
Not a linear pathway, but a complex network
Complexity needs to be modelled in the computer
Computer models of pathways need biochemical kinetic data for every connection.
Enable one to simulate – the change in concentration or– activation (eg. phosphorylation)of the proteins of the pathway
over time.
Modelling gives information on how signals are processed.
The effect of the number of active EGFR molecules on ERK activation
EGFR
PLC Ras PI3K
PKC MAPK PKB/Akt
TFs Functional targets
CELL GROWTH AND PROLIFERATION
ERK
The effect of the number of active EGFR molecules on ERK activation
Schoeberl et al., 2002, Nat. Biotech. 20: 370
500,000 active receptors
50,000 active receptors =
Inhibition by one order of magnitude
EGFR
PLC Ras PI3K
PKC MAPK PKB/Akt
TFs Functional targets
CELL GROWTH AND PROLIFERATION
ERK
The effect of active EGFR number on ERK activation
500,000 active receptors
50,000 active receptors
Can this be achieved by receptor inactivation alone?
The effect of active EGFR number on ERK activation
… Or, what might happen if
• ERK is overexpressed?
• Several proteins in the pathway are abnormally expressed?
The effect of active EGFR number on ERK activation
50,000 active receptors
with normal levels of ERK
or
ERK overexpression and cross-activation
Computer models of pathways• Integration of complex knowledge
– Biological processes are mediated by pathways in health and disease
– Modelling aids integrative understanding of relationships between physiology and clinical observations and the molecular level
• Analysis and simulation of signal processing in cancer cells
– Effects of mutations and abnormal gene expression– Discovery of new targets for therapy: key modulators of pathway
function– Effects of therapeutic inhibitors– Possible side effects
Effects of abnormal gene expression
• Roughly 90% of human cancers are epithelial in origin and exhibit a large number of changes in the structure and function of the genome.
• Abnormal expression levels can be observed for a a large number of genes.
• This complexity might be the reason for the clinical diversity of tumours (even with similar histology).
• A comprehensive analysis of the multiple genetic alterations present is required for an understanding of abnormal signal processing in cancer and differences between tumours.
Gene expression analysis
• The use of expression microarrays enables the large-scale analysis of mRNA expression (expression profiling) in tumour samples.
• Expression profiling can be used to simultaneously
assess the expression of the entire human genome.
• mRNA concentration is used as a surrogate for protein conc. - protein concentrations may be hypothetically inferred.
ER-positive breast tumour subtype has a distinct microarray expression profile
ER = oestrogen receptor
Example: Gene expression profiles from breast cancer patient samples
Role of ER and EGFR in anti-oestrogen therapy
• Response to tamoxifen is dependent on ER expression.
• Overexpression of EGFR is associated with tamoxifen resistance - EGFR as a target for therapy.
• Differences in expression of EGFR and other proteins in the network between patients?
• May account for different responses to therapy with EGFR inhibitors.
ER-positive tumours
genes
EGFR
EGFR as a target for therapy
Modelling of individual response
Gene expression of EGFR network genes in each individual tumour
Approximation of relative changes in protein expression
• Input in computer model
• Model signal processing in different tumours in response to EGFR inhibition
• Hypothesis generation re. response
• Validate with clinical response
Caveat: may be not directly comparable – direct measurement of protein concentration
Summary
Molecular changes in cancer are highly complex.
They affect signal processing in pathways and networks.
Changes in signal processing underpin hallmarks of cancer.
Computer modelling gives information on how signals are processed.
Modelling aids fundamental understanding of cancer, discovery of new targets for therapy, prediction of effects of therapy and possible side effects.