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Discovery of a Drug to Treat a Disease

Medical research on a disease may discover the disease's life cycle.

There may be a critical point in the life cycle that might be disrupted by a drug. E.g. a point where a chemical might bind and prevent the diseases action.

Search space of potential drugs is huge. Estimated $ 10^{40}$ drug like chemicals.

Using high throughput robot based screening in the region of $ 10^{6}$ can be measured.

Computer models are used at many stages of the discovery ``funnel''. They guide chemists as to where to look next.

Models predict as yet unmeasured properties.
They can screen ``virtual'' chemicals, i.e. chemicals that do not exist.
Virtual chemicals could be manufactured, if the computer suggested they might be interesting.

Discovery of a Drug to Treat a Disease

Rat P450 2B1,
Showing cell wall membrane attachment

See.

Why is P450 Important to Drug Discovery

GSK ``Blind Trial''

GSK ``Blind Trial'' Three P450 IC50 data sets

Spread of IC50 in Training Data
IC50 relatively high quality but still noisy data.

Training data was deliberately set up to have equal numbers in each of the three classes.

The test (or interpolation) data set and the extrapolation set very unequal split.

GP Prediction of P450 Inhibition

P450 IC50 Regression

Classification

P450 IC50 training v. test

Best of 5 regression runs and 5 classifications runs are plotted together with best simplified model of both GP approaches.

P450 IC50 (simplified) Regression Model

F1, f2, ... f8 are GSK domain specific features calculated for each chemical from its chemical formula. These 8 features were chosen by GP from the 121 available.

P450 IC50 (simplified) Classification Model


Active


Substrate


Inactive

Each tree yields a value. The tree whose value is largest of the three indicates the predicted class. 21 features were chosen by GP from the 121 available.

GSK Workshop Recommendations

Conclusions


next up previous
Next: About this document ... Up: GP in Drug Discovery Previous: GP in Drug Discovery
Bill LANGDON 2004-02-08