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Section: Application Domains
Precision medicine and pharmacogenomics
Pharmacogenomics involves using an individual's genome to determine whether or not a particular therapy, or dose of therapy, will be effective. Indeed, people's reaction to a given drug depends on their physiological state and environmental factors, but also to their individual genetic make-up.
Precision medicine is an emerging approach for disease treatment and prevention that takes into account individual variability in genes, environment, and lifestyle for each person. While some advances in precision medicine have been made, the practice is not currently in use for most diseases.
Currently, in the traditional population approach, inter-individual variability in the reaction to drugs is modeled using covariates such as weight, age, sex, ethnic origin, etc. Genetic polymorphisms susceptible to modify pharmacokinetic or pharmacodynamic parameters are much harder to include, especially as there are millions of possible polymorphisms (and thus covariates) per patient.
The challenge is to determine which genetic covariates are associated to some PKPD parameters and/or implicated in patient responses to a given drug.
Another problem encountered is the dependence of genes, as indeed, gene expression is a highly regulated process. In cases where the explanatory variables (genomic variants) are correlated, Lasso-type methods for model selection are thwarted.
There is therefore a clear need for new methods and algorithms for the estimation, validation and selection of mixed effects models adapted to the problems of genomic medicine.
A target application of this project concerns the lung cancer.
EGFR (Epidermal Growth Factor Receptor) is a cell surface protein that binds to epidermal growth factor. We know that deregulation of the downstream signaling pathway of EGFR is involved in the development of lung cancers and several gene mutations responsible for this deregulation are known.
Our objective is to identify the variants responsible for the disruption of this pathway using a modelling approach. The data that should be available for developing such model are ERK (Extracellular signal–regulated kinases) phosphorylation time series, obtained from different genetic profiles.
The model that we aim to develop will describe the relationship between the parameters of the pathway and the genomic covariates, i.e. the genetic profile. Variants related to the pathway include: variants that modify the affinity binding of ligands to receptors, variants that modify the total amount of protein, variants that affect the catalytic site,...