Team:Groningen/Modelling/Characterization

From 2009.igem.org

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                   pSB1A2con:    //  concentration mode this is our first icps measerment wild type
                   pSB1A2con:    //  concentration mode this is our first icps measerment wild type
                   {constants:{Vc:0.000808081,Vs:(1-0.000808081),pro:0,ars2T:0},time:Infinity,
                   {constants:{Vc:0.000808081,Vs:(1-0.000808081),pro:0,ars2T:0},time:Infinity,
-
                     data:{AsinT:[0.167289553e-6,0.185086314e-6,0.398647446e-6,0.473393842e-6],
+
                     data:{AsinT:[207.0208222e-6,229.0443139e-6,493.3262146e-6,585.8248799e-6],
                           AsT:[10e-6,20e-6,50e-6,100e-6]}},
                           AsT:[10e-6,20e-6,50e-6,100e-6]}},
                   pSB1A2time:  //  concentration mode this is our first icps measerment wild type
                   pSB1A2time:  //  concentration mode this is our first icps measerment wild type
Line 224: Line 224:
                                 //    We incorporate this in our model by pretending RFP=GVP (1st icps)
                                 //    We incorporate this in our model by pretending RFP=GVP (1st icps)
                   {constants:{Vc:0.001272727,Vs:(1-0.001272727),pro:0},time:Infinity,
                   {constants:{Vc:0.001272727,Vs:(1-0.001272727),pro:0},time:Infinity,
-
                     data:{AsinT:[0.173785371e-6,0.353176722e-6,0.369994661e-6,0.437266418e-6],
+
                     data:{AsinT:[136.5456487e-6,77.4959957e-6,290.7100908e-6,343.5664709e-6],
                           AsT:[10e-6,20e-6,50e-6,100e-6]}},
                           AsT:[10e-6,20e-6,50e-6,100e-6]}},
                   pArsRRFPtime:  // here the cell only contains extra RFP behind the the extra ArsR promotors.
                   pArsRRFPtime:  // here the cell only contains extra RFP behind the the extra ArsR promotors.

Revision as of 10:59, 13 October 2009

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TODO: Talk about the devices we have and in what way we want to characterize them.

Uptake measurements

Sampling scheme
Time (min)
0 10 20 40 60
As(III)exT(0)
(µM) 		0 x
10 x x x x x
20 x
50 x
100 x

To efficiently look at both time and concentration dependent processes we took samples as in the table on the right. Below we list all results, which have been used for fitting all necessary parameters.

TODO: List results. Take conversion from nmol/mg and mg/ml to µM and Vc/Vs into account.

best cur gradient solved
v5/K5
v5
K5
k8/K7
k8
K7
tauBbeta4
tauB
beta4
tauR
beta1
tauFbetaF
tauF
betaF
tauKbetaK
tauK
betaK
tauGbeta5
tauG
beta5
E

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