Team:Grenoble/Biology/Network

From 2012.igem.org

(Difference between revisions)
Line 12: Line 12:
<a href="https://2012.igem.org/Team:Grenoble/Biology/Network#20" class="schema" ><img src="https://static.igem.org/mediawiki/2012/b/bb/Circuit2.png" alt="" style="position: relative; top: 54px;" /></a>
<a href="https://2012.igem.org/Team:Grenoble/Biology/Network#20" class="schema" ><img src="https://static.igem.org/mediawiki/2012/b/bb/Circuit2.png" alt="" style="position: relative; top: 54px;" /></a>
<a href="https://2012.igem.org/Team:Grenoble/Biology/Network#10" class="schema" ><img src="https://static.igem.org/mediawiki/2012/a/a4/Circuit_gre.png" alt="" style="position: relative; top: -468px;"/></a>
<a href="https://2012.igem.org/Team:Grenoble/Biology/Network#10" class="schema" ><img src="https://static.igem.org/mediawiki/2012/a/a4/Circuit_gre.png" alt="" style="position: relative; top: -468px;"/></a>
-
 
-
<section style="position: relative; top: -80px;">
 
</section>
</section>
-
<section>
+
<section style="position: relative; top: -80px;">
 +
 
<h2 id="10">Signaling module</h2>
<h2 id="10">Signaling module</h2>

Revision as of 22:27, 23 September 2012

iGEM Grenoble 2012

iGEM Grenoble iGEM
iGEM 2012
main page
Project

Network details

Our system is divided in two modules:
  • signaling module
  • amplification module

Signaling module

The signaling module allows our bacterial strain to integrate the input signal = the pathogene presence.

Stapylococcus aureus secrete a protease nom de la protéase which cut a specific amino-acids sequence. This specific sequence can be used as a linker between a membrane protein and a dipeptide.
Once S. aureus is present, the linker is cut by the protease and the dipeptide is released.

The dipeptide binds to his receptor which is an engineered receptor:
  • the extracellular part is the extracellular part of Tap, a dipeptide receptor involved in the chemotaxism
  • the intracellular part is the intracellular part of EnvZ, a kinase involved in the osmoregulation

Once the dipeptide is bound, the EnvZ part allows the phosphorylation of OmpR, a transcriptional activator.

Amplification module

The amplification module allows our bacterial strain to amplify the input signal and to produce an output signal = fluorescence.

Once OmpR is phosphorylated, it allows the production of adenyl cyclase by activating the OmpC promoter.
Adenyl cyclase is an enzyme which catalyse the conversion of ATP (Adenosine Tri-Phosphate) to cAMP (cyclic Adenosine Mono-Phosphate).


cAMP binds to CRP (C-reactive protein) and then this complex allows the production of AraC by activating pMalT promoter.
In the presence of arabinose, AraC, with cAMP-CRP, activates the pAraBAD promoter which allow the production of:
  • adenyl cyclase which reproduce cAMP forming an amplification loop
  • GFP (Green Fluorescent Protein) = our output signal

Retrieved from "http://2012.igem.org/Team:Grenoble/Biology/Network"