Team:Leeds/Modeling
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We plan to use modelling to help test and characterise our Bio-Devices. This includes modelling our expected fluorescence based upon Fluorescent Protein production, statistical modelling and testing for physical binding versus false positives and various other parts of the project. | We plan to use modelling to help test and characterise our Bio-Devices. This includes modelling our expected fluorescence based upon Fluorescent Protein production, statistical modelling and testing for physical binding versus false positives and various other parts of the project. | ||
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Revision as of 22:02, 4 October 2013
We plan to use modelling to help test and characterise our Bio-Devices. This includes modelling our expected fluorescence based upon Fluorescent Protein production, statistical modelling and testing for physical binding versus false positives and various other parts of the project.
Modelling The Cpx PathwayThe key to making MicroBeagle successful hinges on proper integration with the Cpx pathway. As such, it is essential we develop a god working model, not only to predict how much fluorescence we can expect in different environments, but also to prototype and test potential methods for controlling this; in turn reducing our false positive rate.
Cpx Pathway ModelDue to the high complexity of the Cpx Pathway, it was necessary to graphically plot the processes taking place within the cell by hand, allowing us to then simplify and compartmentalize aspects which, while having an effect on the overall results, were of no interest to us. The above image shows the 3rd iteration of this, with colour-coded interactions, products and proteins. The main enzymes of interest were specifically named, while a general product labelled as 'denaturants' was listed to encompass the more than 100 other Cpx-mediated protein syntheses. This would be inaccurate, if not for the use of Rules-Based software, such as RuleBender - for the model to work, one must list the starting concentrations of each molecular species, hence by setting the 'denaturant' promoter concentration to be at least 100 times greater than that of pGFP or pCpxP, the relative interaction mechanics are preserved. | |||||||
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