ETHZ/Parameters

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Revision as of 12:10, 13 October 2007

Introduction

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Model Parameters

Parameter	Value	Description	Comments	Parameter	Value	Description	Comments
c₁^max	0.01 [mM/h]	max. transcription rate of constitutive promoter (per gene)	promoter no. J23105; Reference: Estimate	c₂^max	0.01 [mM/h]	max. transcription rate of luxR-activated promoter (per gene)	Reference: Estimate
l^hi	25	high-copy plasmid number	Reference: Estimate	l^lo	5	low-copy plasmid number	Reference: Estimate
a_Q₂,R	0.1 - 0.2	basic production of Q₂/R-inhibited genes	Reference: Conclusions after discussion	a_Q₂	0.1 - 0.2	basic production of Q₂-inhibited genes	Reference: Conclusions after discussion
a_Q₁,S	0.1 - 0.2	basic production of Q₁/S-inhibited genes	Reference: Conclusions after discussion	a_Q₁	0.1 - 0.2	basic production of Q₁-inhibited genes	Reference: Conclusions after discussion
a_Q₂,S	0.1 - 0.2	basic production of Q₂/S-inhibited genes	Reference: Conclusions after discussion	a_Q₁,R	0.1 - 0.2	basic production of Q₁/R-inhibited genes	Reference: Conclusions after discussion
Degradation constants
d_R	2.31e-3 [per sec]	degradation of lacI	Ref. [10]	d_S	1e-5 [pro sec]/2.31e-3 [per sec]	degradation of tetR	Ref. [9]/ Ref. [10]
d_L	1e-3 - 1e-4 [per sec]	degradation of luxR	Ref: [6]
d_Q₁	7e-4 [per sec]	degradation of cI	Ref. [7]	d_Q₂		degradation of p22cII
d_YFP	6.3e-3 [per min]	degradation of YFP	suppl. mat. to Ref. [8] corresponding to a half life of 110min	d_GFP	6.3e-3 [per min]	degradation of GFP	in analogy to YFP
d_RFP	6.3e-3 [per min]	degradation of RFP	in analogy to YFP	d_CFP	6.3e-3 [per min]	degradation of CFP	in analogy to YFP
Dissociation constants
K_R	0.1 - 1 [pM]	lacI repressor dissociation constant	Ref. [2]	K_{I_R}	1.3 [µM]	IPTG-lacI repressor dissociation constant	Ref. [2]
K_S	179 [pM]	tetR repressor dissociation constant	Ref. [1]	K_{I_S}	893 [pM]	aTc-tetR repressor dissociation constant	Ref. [1]
K_L	55 - 520 [nM]	luxR activator dissociation constant	Ref: [6]	K_{I_L}	0.09 - 1 [µM]	AHL-luxR activator dissociation constant	Ref: [6]
K_Q₁	8 [pM] 50 [nM]	cI repressor dissociation constant	Ref. [12] starting with values of Ref. [6] and using Ref. [3]	K_Q₂	0.577 [µM]	p22cII repressor dissociation constant	Ref. [11]. Note that they use a protein cII and we have p22cII. Does that match?
Hill cooperativity
n_R	1	lacI repressor Hill cooperativity	Ref. [5]	n_{I_R}	2	IPTG-lacI repressor Hill cooperativity	Ref. [5]
n_S	3	tetR repressor Hill cooperativity	Ref. [3]	n_{I_S}	2 (1.5-2.5)	aTc-tetR repressor Hill cooperativity	Ref. [3]
n_L	2	luxR activator Hill cooperativity	Ref: [6]	n_{I_L}	1	AHL-luxR activator Hill cooperativity	Ref. [3]
n_Q₁	2	cI repressor Hill cooperativity	Ref. [12]	n_Q₂	4	p22cII repressor Hill cooperativity	Ref. [11]. Note that they use a protein cII and we have p22cII. Does that match?

Parameter	Value	Description	Comments		Parameter	Value	Description	Comments
c₁^max	0.01 [mM/h]	max. transcription rate of constitutive promoter (per gene)	promoter no. J23105; Reference: Estimate		c₁^max	0.01 [mM/h]	max. transcription rate of constitutive promoter (per gene)	promoter no. J23105; Reference: Estimate

Hill cooperativity

Parameter	Value	Description	Comments
c₁^max	0.01 [mM/h]	max. transcription rate of constitutive promoter (per gene)	promoter no. J23105; Reference: Estimate
c₂^max	0.01 [mM/h]	max. transcription rate of luxR-activated promoter (per gene)	Reference: Estimate
l^hi	25	high-copy plasmid number	Reference: Estimate
l^lo	5	low-copy plasmid number	Reference: Estimate
a_Q₂,R	0.1 - 0.2	basic production of Q₂/R-inhibited genes	Reference: Conclusions after discussion
a_Q₂	0.1 - 0.2	basic production of Q₂-inhibited genes	Reference: Conclusions after discussion
a_Q₁,S	0.1 - 0.2	basic production of Q₁/S-inhibited genes	Reference: Conclusions after discussion
a_Q₁	0.1 - 0.2	basic production of Q₁-inhibited genes	Reference: Conclusions after discussion
a_Q₂,S	0.1 - 0.2	basic production of Q₂/S-inhibited genes	Reference: Conclusions after discussion
a_Q₁,R	0.1 - 0.2	basic production of Q₁/R-inhibited genes	Reference: Conclusions after discussion
d_R	2.31e-3 [per sec]	degradation of lacI	Ref. [10]
d_S	1e-5 [pro sec]/2.31e-3 [per sec]	degradation of tetR	Ref. [9]/ Ref. [10]
d_L	1e-3 - 1e-4 [per sec]	degradation of luxR	Ref: [6]
d_Q₁	7e-4 [per sec]	degradation of cI	Ref. [7]
d_Q₂		degradation of p22cII
d_YFP	6.3e-3 [per min]	degradation of YFP	suppl. mat. to Ref. [8] corresponding to a half life of 110min
d_GFP	6.3e-3 [per min]	degradation of GFP	in analogy to YFP
d_RFP	6.3e-3 [per min]	degradation of RFP	in analogy to YFP
d_CFP	6.3e-3 [per min]	degradation of CFP	in analogy to YFP
K_R	0.1 - 1 [pM]	lacI repressor dissociation constant	Ref. [2]
K_{I_R}	1.3 [µM]	IPTG-lacI repressor dissociation constant	Ref. [2]
K_S	179 [pM]	tetR repressor dissociation constant	Ref. [1]
K_{I_S}	893 [pM]	aTc-tetR repressor dissociation constant	Ref. [1]
K_L	55 - 520 [nM]	luxR activator dissociation constant	Ref: [6]
K_{I_L}	0.09 - 1 [µM]	AHL-luxR activator dissociation constant	Ref: [6]
K_Q₁	8 [pM] 50 [nM]	cI repressor dissociation constant	Ref. [12] starting with values of Ref. [6] and using Ref. [3]
K_Q₂	0.577 [µM]	p22cII repressor dissociation constant	Ref. [11]. Note that they use a protein cII and we have p22cII. Does that match?
n_R	1	lacI repressor Hill cooperativity	Ref. [5]
n_{I_R}	2	IPTG-lacI repressor Hill cooperativity	Ref. [5]
n_S	3	tetR repressor Hill cooperativity	Ref. [3]
n_{I_S}	2 (1.5-2.5)	aTc-tetR repressor Hill cooperativity	Ref. [3]
n_L	2	luxR activator Hill cooperativity	Ref: [6]
n_{I_L}	1	AHL-luxR activator Hill cooperativity	Ref. [3]
n_Q₁	2	cI repressor Hill cooperativity	Ref. [12]
n_Q₂	4	p22cII repressor Hill cooperativity	Ref. [11]. Note that they use a protein cII and we have p22cII. Does that match?

References

[http://www.pnas.org/cgi/content/abstract/104/8/2643 [1] Weber W et al.] "A synthetic time-delay circuit in mammalian cells and mice", P Natl Acad Sci USA 104(8):2643-2648, 2007
[http://www.pnas.org/cgi/content/full/100/13/7702?ck=nck [2] Setty Y et al.] "Detailed map of a cis-regulatory input function", P Natl Acad Sci USA 100(13):7702-7707, 2003
[http://ieeexplore.ieee.org/iel5/9711/30654/01416417.pdf [3] Braun D et al.] "Parameter Estimation for Two Synthetic Gene Networks: A Case Study", ICASSP 5:769-772, 2005
[http://www.nature.com/nature/journal/v435/n7038/suppinfo/nature03508.html [4] Fung E et al.] "A synthetic gene--metabolic oscillator", Nature 435:118-122, 2005 (supplementary material)
[http://dx.doi.org/10.1016/j.jbiotec.2005.08.030 [5] Iadevaia S and Mantzais NV] "Genetic network driven control of PHBV copolymer composition", J Biotechnol 122(1):99-121, 2006
[http://dx.doi.org/10.1016/j.biosystems.2005.04.006 [6] Goryachev AB et al.] "Systems analysis of a quorum sensing network: Design constraints imposed by the functional requirements, network topology and kinetic constants", Biosystems 83(2-3):178-187, 2004
[http://www.genetics.org/cgi/content/abstract/149/4/1633 [7] Arkin A et al.] "Stochastic kinetic analysis of developmental pathway bifurcation in phage λ-Infected Escherichia coli cells", Genetics 149: 1633-1648, 1998
[http://download.cell.com/supplementarydata/cell/107/6/739/DC1/index.htm [8] Colman-Lerner A et al.] "Yeast Cbk1 and Mob2 Activate Daughter-Specific Genetic Programs to Induce Asymmetric Cell Fates", Cell 107(6): 739-750, 2001 (supplementary material)
[http://www.nature.com/nature/journal/v405/n6786/abs/405590a0.html [9] Becskei A and Serrano L] "Engineering stability in gene networks by autoregulation", Nature 405: 590-593, 2000
[http://www.biophysj.org/cgi/content/full/89/6/3873?maxtoshow=&HITS=10&hits=10&RESULTFORMAT=&searchid=1&FIRSTINDEX=0&volume=89&firstpage=3873&resourcetype=HWCIT [10] Tuttle et al.] "Model-Driven Designs of an Oscillating Gene Network", Biophys J 89(6):3873-3883, 2005
[http://www.pnas.org/cgi/reprint/99/2/679 [11] McMillen LM et al.] "Synchronizing genetic relaxation oscillators by intercell signaling", P Natl Acad Sci USA 99(2):679-684, 2002
[http://www.nature.com/nature/journal/v434/n7037/full/nature03461.html [12] Basu S et al.] "A synthetic multicellular system for programmed pattern formation", Nature 434:1130-1134, 2005

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 | Ref: [6]
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 | d<sub>Q<sub>1</sub></sub>
 | 7e-4 [per sec]
 | degradation of cI
 | Ref. [7]
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 | d<sub>Q<sub>2</sub></sub>
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 | degradation of p22cII
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 | d<sub>YFP</sub>
 | 6.3e-3 [per min]
 | degradation of YFP
 | suppl. mat. to Ref. [8] corresponding to a half life of 110min
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 | d<sub>GFP</sub>
 | 6.3e-3 [per min]
 | degradation of GFP
 | in analogy to YFP
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 | d<sub>RFP</sub>
 | 6.3e-3 [per min]
 | degradation of RFP
 | in analogy to YFP
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 | d<sub>CFP</sub>
 | 6.3e-3 [per min]
 | degradation of CFP
 | in analogy to YFP
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+| Dissociation constants
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 | K<sub>R</sub>
 | 0.1 - 1 [pM]
 | lacI repressor dissociation constant
 | Ref. [2]
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 | K<sub>I<sub>R</sub></sub>
 | 1.3 [&#181;M]
 | IPTG-lacI repressor dissociation constant
 | Ref. [2]
-|
+|-
 | K<sub>S</sub>
 | 179 [pM]
 | tetR repressor dissociation constant
 | Ref. [1]
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 | K<sub>I<sub>S</sub></sub>
 | 893 [pM]
 | aTc-tetR repressor dissociation constant
 | Ref. [1]
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+|-
 | K<sub>L</sub>
 | 55 - 520 [nM]
 | luxR activator dissociation constant
 | Ref: [6]
-|-
+|
 | K<sub>I<sub>L</sub></sub>
 | 0.09 - 1 [&#181;M]
 | AHL-luxR activator dissociation constant
 | Ref: [6]
-|
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 | K<sub>Q<sub>1</sub></sub>
 |
@@ Line 160: / Line 175: @@
 * Ref. [12]
 * starting with values of Ref. [6] and using Ref. [3]
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 | K<sub>Q<sub>2</sub></sub>
 | 0.577 [&#181;M]
 | p22cII repressor dissociation constant
 | Ref. [11]. Note that they use a protein cII and we have p22cII. Does that match?
+|-
+|Hill cooperativity
 |
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 | n<sub>R</sub>
 | 1
 | lacI repressor Hill cooperativity
 | Ref. [5]
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 | n<sub>I<sub>R</sub></sub>
 | 2
 | IPTG-lacI repressor Hill cooperativity
 | Ref. [5]
-|
+|-
 | n<sub>S</sub>
 | 3
 | tetR repressor Hill cooperativity
 | Ref. [3]
-|-
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 | n<sub>I<sub>S</sub></sub>
 | 2 (1.5-2.5)
 | aTc-tetR repressor Hill cooperativity
 |Ref. [3]
-|
+|-
 | n<sub>L</sub>
 | 2
 | luxR activator Hill cooperativity
 | Ref: [6]
-|-
+|
 | n<sub>I<sub>L</sub></sub>
 | 1
 | AHL-luxR activator Hill cooperativity
 | Ref. [3]
-|
+|-
 | n<sub>Q<sub>1</sub></sub>
 | 2
 | cI repressor Hill cooperativity
 | Ref. [12]
-|-
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 | n<sub>Q<sub>2</sub></sub>
 | 4
@@ Line 378: / Line 403: @@
 | p22cII repressor dissociation constant
 | Ref. [11]. Note that they use a protein cII and we have p22cII. Does that match?
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+Hill cooperativity
 |-
 | n<sub>R</sub>