Team:ULB-Brussels/Safety
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- | <p>In the current state of our project, the protein production is boosted thanks to a TA system, but the plasmids are maintained through the usual system of antibiotic resistance, since the toxin and the antitoxin will be placed on different plasmids bearing different resistance genes. The system will thus decay quickly if $\MyColi$ bacteria wander in a wild environment, without any antibiotic. In the final version of our project (that is, if we have the time to go this far), the toxin gene will be inserted in the genomic DNA of the bacteria, preventing it to ever be lost, and compelling the bacteria to keep the plasmid bearing the antitoxin and the protein of interest genes. It will also prevent any reasonable chance of | + | <p>In the current state of our project, the protein production is boosted thanks to a TA system, but the plasmids are maintained through the usual system of antibiotic resistance, since the toxin and the antitoxin will be placed on different plasmids bearing different resistance genes. The system will thus decay quickly if $\MyColi$ bacteria wander in a wild environment, without any antibiotic. In the final version of our project (that is, if we have the time to go this far), the toxin gene will be inserted in the genomic DNA of the bacteria, preventing it to ever be lost, and compelling the bacteria to keep the plasmid bearing the antitoxin and the protein of interest genes. It will also prevent any reasonable chance of HGT of the $\MyColi$ System.</p> |
<p>If, for one reason or another, the overproduction of a protein did not results in a competitive disadvantage, it would be wise to implement a build-in suicide sequence in the bacteria, to prevent it surviving outside the bioreactor. It can easily be done by the subordination of the antitoxin production to an inducible promoter that would be activated by a compound only present in the bioreactor. Several of containment devices have been developed by iGEM teams and other are already in use in the industry.</p> | <p>If, for one reason or another, the overproduction of a protein did not results in a competitive disadvantage, it would be wise to implement a build-in suicide sequence in the bacteria, to prevent it surviving outside the bioreactor. It can easily be done by the subordination of the antitoxin production to an inducible promoter that would be activated by a compound only present in the bioreactor. Several of containment devices have been developed by iGEM teams and other are already in use in the industry.</p> | ||
Revision as of 07:51, 11 September 2014
$~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~ \newcommand{\MyColi}{{\small Mighty\hspace{0.12cm}Coli}} \newcommand{\Stabi}{\small Stabi}$ $\newcommand{\EColi}{\small E.coli} \newcommand{\SCere}{\small S.cerevisae}\\[0cm] ~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~~ \newcommand{\PI}{\small PI}$ $\newcommand{\Igo}{\Large\mathcal{I}} \newcommand{\Tgo}{\Large\mathcal{T}} \newcommand{\Ogo}{\Large\mathcal{O}} ~$
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