Team:ETH Zurich/Modeling/Overview
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'''Results:''' <br> | '''Results:''' <br> | ||
- | The property of | + | The property of restriction enzymes are all related to their frequency of cutting. The mean number of genes for fragments as well as its variance and the probability of containing essential genes can be derived only from frequency information.<br><br> |
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The state-of-the-art genome scale model for E.Coli iAF1260 (1260 genes included) was modified in order to account for thymidine auxotrophycity, thymidine uptaking limitation, genome reduction and growth on different medium. Stochastic algorithm and flux balance analysis were applied to predict growth rates.<br><br> | The state-of-the-art genome scale model for E.Coli iAF1260 (1260 genes included) was modified in order to account for thymidine auxotrophycity, thymidine uptaking limitation, genome reduction and growth on different medium. Stochastic algorithm and flux balance analysis were applied to predict growth rates.<br><br> | ||
'''Results:''' <br> | '''Results:''' <br> | ||
- | + | Models show that is indeed possible to select reduced genome strains using thymidine limitation. The quantification shows that the method is at the border line with the sensitivity of chemostat machinery setup fro small reductions, effective for big reductions. Predictions shows the possibility of reducing up to X % of genes for a minimal medium growing strains and Y % of genes for rich medium growing strains.<br><br> | |
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Revision as of 14:51, 25 October 2008
Overview on the modelling frameworkThis page is meant to give an introduction to the the overall modelling framework we have constructed in order to asses feasibility analysis, temporal scale details and other parameter estimations that regard our project setup. As introduced in the project overview section, four main components can be identified in the devised mechanism. Accordingly, we divided the modelling framework in four modules that tack the relative problematics.
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