Difference between revisions of "Team:Aalto-Helsinki/Car-activation"
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<h2>Model</h2> | <h2>Model</h2> | ||
− | <p>The reaction transforming Car from its inactive (called | + | <p>The reaction transforming Car from its inactive (called Car\(_\text{apo}\)) form into its active (called Car\(_\text{holo}\)) form is as follows:</p> |
<p style="color:gray;">--Formulas of the reactions here, need checking!!--</p> | <p style="color:gray;">--Formulas of the reactions here, need checking!!--</p> | ||
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</table> | </table> | ||
− | <p>We modeled the creation of | + | <p>We modeled the creation of Car\(_\text{apo}\) as a constant flux reaction and the degradation of different proteins as a reaction abiding the laws of mass action. This is because we assume we aren’t affecting the DNA transcription and translation in our model and since protein degradation is an enzymatic reaction that is hard to model we simplify it as a mass-action reaction.</p> |
</section> | </section> | ||
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</figure> | </figure> | ||
− | <p>The amount of active Car in the system varies with the enzyme degradation and creation rates. Within this variation the values that the relation | + | <p>The amount of active Car in the system varies with the enzyme degradation and creation rates. Within this variation the values that the relation Car\(_\text{holo}\)/Car got are between 90% and 100%.</p> |
<p style="margin-bottom:0;padding-bottom:10%;">There are some weak points to this model: Since we could not get data about DNA transcription and translation speed, this model is mainly used to find lower limits for the amount of active Car we have in our cells. Also, it might be wrong to assume that a cell reaches equilibrium in its enzymes’ amounts. However, this model shows that unless enzymes are created and degraded with awe-inspiring speeds our system will have most of its Car enzyme in the active form. In fact, according to this model, Car would need to be created and degraded with a speed of 20 µM/min for us to have 50% of Car active. When we compare this with the fact that we only have about 1 µM of Car in our cell, we can safely say that in most scenarios our Car is mostly if not entirely in its active form.</p> | <p style="margin-bottom:0;padding-bottom:10%;">There are some weak points to this model: Since we could not get data about DNA transcription and translation speed, this model is mainly used to find lower limits for the amount of active Car we have in our cells. Also, it might be wrong to assume that a cell reaches equilibrium in its enzymes’ amounts. However, this model shows that unless enzymes are created and degraded with awe-inspiring speeds our system will have most of its Car enzyme in the active form. In fact, according to this model, Car would need to be created and degraded with a speed of 20 µM/min for us to have 50% of Car active. When we compare this with the fact that we only have about 1 µM of Car in our cell, we can safely say that in most scenarios our Car is mostly if not entirely in its active form.</p> |
Revision as of 15:36, 13 September 2015