Difference between revisions of "Team:NTU-LIHPAO-Taiwan/Modeling/Conclusion"
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<li><a href="https://2015.igem.org/Team:NTU-LIHPAO-Taiwan/Description">Description</a></li> | <li><a href="https://2015.igem.org/Team:NTU-LIHPAO-Taiwan/Description">Description</a></li> | ||
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<li><a href="https://2015.igem.org/Team:NTU-LIHPAO-Taiwan/Composite_Part">Composite Parts</a></li> | <li><a href="https://2015.igem.org/Team:NTU-LIHPAO-Taiwan/Composite_Part">Composite Parts</a></li> | ||
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<div class="Text1">Modeling Summary</div> | <div class="Text1">Modeling Summary</div> | ||
− | <div class="Text2" id=" | + | <div class="Text2" id="First1">Hypothesis</div> |
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− | <li> | + | <li>Total oral ingestion of 10<sup>9</sup> <i>L. casei</i> on the first day.</li> |
− | <li> | + | <li>The varying ratio (%) of bacteria number to total ingested number attached on the intestine against time were according to the mouse experiment.</li> |
− | <li> | + | <li>Incorporate suicide mechanism: 4 days for bacteria survival.</li> |
− | <li> | + | <li>TAT penetrates through villi by an uncharacterized pinocytosis/endocytosis related mechanism, which is also receptor-independent.</li> |
− | <li> | + | <li>CPP-PYY complex production rate per <i>L. casei</i> : 10<sup>-10</sup> μg/min.</li> |
− | <li> | + | <li>One-fourth of the products secreted from <i>L. casei</i> penetrate through the small intestine epithelial cells, without being digested by the intestine fluid.</li> |
− | <li> | + | <li>Effective permeability of TAT-insulin conjugates from literature as reference for TAT-PYY complex : P<sub>eff</sub> = 1.62×10<sup>-5</sup> (cm/s).</li> |
− | <li> | + | <li>Mean total mucosal surface of the small intestine interior averages 32 m<sup>2</sup>.</li> |
− | <li> | + | <li><i>L. casei</i> cell size range = 0.7-1.1 x 2.0-4.0 μm. One-tenth of the bacteria height multiplied the mucosa surface area for the donor chamber volume.</li> |
− | <li> | + | <li>Fick’s Law of Binary Diffusion applied for CPP-PYY complex adsorption into bloodstream. Interstitial fluid diffusion coefficient of bovine serum albumin in tissues was taken for reference : D<sub>AB</sub> = 5.8 x 10<sup>-7</sup> cm<sup>2</sup>/s.</li> |
+ | <li>The distance from epithelial cells to capillaries is 4 μm.</li> | ||
+ | <li>The diffusion is rapid enough to adsorb all the products in every minute.</li> | ||
+ | <li>All the calculation was based on reaching steady-state condition in the interval of every minute discretely.</li> | ||
+ | <li>Thrombin cleavage efficiency of Arg-Ser(R-S) site in CPP-PYY complex was referred to Arg-Thr(R-T) site in salmon calcitonin.</li> | ||
+ | <li>Nearly 100 % of the complexes would be cleaved during 30 minutes due to the fluid motion in circulation.</li> | ||
+ | <li>PYY concentration of 100 pg/ml has the power of appetite suppression without drug resistance.</li> | ||
+ | <li>Average total blood volume of 5 liter in human body.</li> | ||
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− | <div class="Text2" id=" | + | <div class="Text2" id="First2">Conclusion</div> |
<div class="Text3"> | <div class="Text3"> | ||
Ideally, the optimal concentration of PYY is 0.1 μg/L for appetite suppression, giving little side effect. Here we performed the simulation with 10<sup>9</sup> of total <i>L. casei</i> intake, and 10<sup>-10</sup> μg/min of CPP-PYY complex production rate per <i>L. casei</i>. The results is shown below. | Ideally, the optimal concentration of PYY is 0.1 μg/L for appetite suppression, giving little side effect. Here we performed the simulation with 10<sup>9</sup> of total <i>L. casei</i> intake, and 10<sup>-10</sup> μg/min of CPP-PYY complex production rate per <i>L. casei</i>. The results is shown below. | ||
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<img src="https://static.igem.org/mediawiki/2015/d/de/Pathway_Figure7.png" width="500px"/> | <img src="https://static.igem.org/mediawiki/2015/d/de/Pathway_Figure7.png" width="500px"/> | ||
− | <div class="Article_PictureText1"><div class="Text_Picture">[Fig. | + | <div class="Article_PictureText1"><div class="Text_Picture">[Fig.2-1] Final concentration of PYY (μg/L) in the blood vessel</div></div> |
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This general formula is based on one-dose response, and continuous drug intake should be further modified by successive accumulation for determining the appetite suppression effect. | This general formula is based on one-dose response, and continuous drug intake should be further modified by successive accumulation for determining the appetite suppression effect. | ||
</div> | </div> | ||
− | + | <div class="Text3"> | |
− | + | <b>—></b> <a href="https://2015.igem.org/Team:NTU-LIHPAO-Taiwan/Modeling"><b>[Click on here back to Modeling Introduction]</b></a> | |
− | + | </div> | |
− | + | <div class="Text3"> | |
− | + | <b>—></b> <a href="https://2015.igem.org/Team:NTU-LIHPAO-Taiwan/Modeling/Conclusion"><b>[Click on here to see our Simulation Strategy and Results]</b></a> | |
− | + | </div> | |
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Latest revision as of 13:17, 18 September 2015
- Modeling Summary
Modeling Summary
Hypothesis
- Total oral ingestion of 109 L. casei on the first day.
- The varying ratio (%) of bacteria number to total ingested number attached on the intestine against time were according to the mouse experiment.
- Incorporate suicide mechanism: 4 days for bacteria survival.
- TAT penetrates through villi by an uncharacterized pinocytosis/endocytosis related mechanism, which is also receptor-independent.
- CPP-PYY complex production rate per L. casei : 10-10 μg/min.
- One-fourth of the products secreted from L. casei penetrate through the small intestine epithelial cells, without being digested by the intestine fluid.
- Effective permeability of TAT-insulin conjugates from literature as reference for TAT-PYY complex : Peff = 1.62×10-5 (cm/s).
- Mean total mucosal surface of the small intestine interior averages 32 m2.
- L. casei cell size range = 0.7-1.1 x 2.0-4.0 μm. One-tenth of the bacteria height multiplied the mucosa surface area for the donor chamber volume.
- Fick’s Law of Binary Diffusion applied for CPP-PYY complex adsorption into bloodstream. Interstitial fluid diffusion coefficient of bovine serum albumin in tissues was taken for reference : DAB = 5.8 x 10-7 cm2/s.
- The distance from epithelial cells to capillaries is 4 μm.
- The diffusion is rapid enough to adsorb all the products in every minute.
- All the calculation was based on reaching steady-state condition in the interval of every minute discretely.
- Thrombin cleavage efficiency of Arg-Ser(R-S) site in CPP-PYY complex was referred to Arg-Thr(R-T) site in salmon calcitonin.
- Nearly 100 % of the complexes would be cleaved during 30 minutes due to the fluid motion in circulation.
- PYY concentration of 100 pg/ml has the power of appetite suppression without drug resistance.
- Average total blood volume of 5 liter in human body.
Conclusion
Ideally, the optimal concentration of PYY is 0.1 μg/L for appetite suppression, giving little side effect. Here we performed the simulation with 109 of total L. casei intake, and 10-10 μg/min of CPP-PYY complex production rate per L. casei. The results is shown below.
[Fig.2-1] Final concentration of PYY (μg/L) in the blood vessel
By building the model for simulation step by step, we summarized the general formula with varies parameters to determine the dose response :
[Final concentration of PYY in the blood (μg/L)] = 11745 × [Total L. casei intake] × [Distribution ratio of L. casei] × [CPP-PYY complex production rate per L. casei (μg/min)]
This general formula is based on one-dose response, and continuous drug intake should be further modified by successive accumulation for determining the appetite suppression effect.
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