Difference between revisions of "Team:Tianjin/Model"

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                                         Oscillation in KaiC phosphorylation is the best-observed parameter in this system and represents a key state variable for the clock in vivo. Thus we have sought to closely mimic this output in our project. Nakajima et al. <sup><a href="#re6">[6]</a></sup> suggest, given the dual function of KaiC and ‘‘cooperation between KaiA and KaiB,’’ that autonomous oscillation of KaiC phosphorylation might be achieved. We established a model based on known biological and biochemical observations and our experiments that did not involve transcription or translation. In <a href="#14">Figure14</a>, we summarized the key steps of three Kai proteins oscillation when ATP is provided in excess. It was well established that we used three circles to represent all possible combinations of three Kai proteins, just like Mars and its two satellites. This was also why we call it Mars Model.
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                                         Oscillation in KaiC phosphorylation is the best-observed parameter in this system and represents a key state variable for the clock in vivo. Thus we have sought to closely mimic this output in our project. Nakajima et al. <sup><a href="#re6">[6]</a></sup> suggest, given the dual function of KaiC and ‘‘cooperation between KaiA and KaiB,’’ that autonomous oscillation of KaiC phosphorylation might be achieved. We established a model based on known biological and biochemical observations and our experiments that did not involve transcription or translation. In <a href="#14">Figure14</a>, we summarized the key steps of three Kai proteins oscillation when ATP is provided in excess. It was well established that we used three circles to represent all possible combinations of three Kai proteins, just like Mars and its two satellites. This was also why we call it <b>Mars Model</b>.
 
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Revision as of 02:33, 18 October 2018

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MODEL

Overview

The models we built included four parts. First, we established a fluorescent protein model to screen out the most suitable fluorescent protein, the main modeling method here is grayscale analysis. Then, for the large amount of measured OD values, we drew the growth curve of yeasts and it fitted logistic model. It described the growth situation of the yeasts after plasmid introduction, and we compare it with yeasts without any foreign plasmid. The growth curve also offers the best measuring point and the best measuring interval. What’s more, we drew the degradation curve of the fluorescent protein, which helps us know different characteristics of the two chosen fluorescent proteins better. Finally, we constructed a model to illustrate the oscillation of KaiA, KaiB and KaiC protein called Mars Model, it explained the reason why the cycle reduced in yeasts nicely. Modeling work integrated with experiments tightly made our project complete and convincing.