Team:Grenoble/Modeling/Amplification
From 2012.igem.org
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- | In this part we will model the amplification module. Our work in this module is subdivided in three main parts: a deterministic model of the reactions at the local scale, another version of the former taking into account | + | In this part we will model the amplification module. Our work in this module is subdivided in three main parts: a deterministic model of the reactions at the local scale, another version of the former taking into account random noise and perturbations, and a model including diffusion in space and time. |
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- | In the deterministic model, we | + | In the deterministic model, we determine the sensitivity of our system and we link it to the signaling module. Then, in the diffusion part we check if our system has a fast answer. Eventually, in the random perturbations model, we check that it is robust to perturbations. |
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<h1> Overview</h1> | <h1> Overview</h1> | ||
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- | The protein GFP is | + | The protein GFP is a reporter protein for adenylate cyclase. Thus, in the development, gfp will be omitted, and we will consider that the adenylate cyclase gives us the signal. |
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<b>Why an amplification module?</b> | <b>Why an amplification module?</b> | ||
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- | + | How to do this? | |
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- | First, we | + | First, we chose a molecule, which is produced by bacteria and diffuses from bacteria to the other bacterium. We chose cyclic AMP, whose production is catalyzed by the adenylate cyclase. Thus, we designed: |
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Latest revision as of 02:57, 27 September 2012